Your search keyword '"Stoler, P."' showing total 40 results

1. Accurate sequencing of DNA motifs able to form alternative (non-B) structures.

Author

Eckert, Kristin, Chiaromonte, Francesca, Huang, Yi-Fei, Makova, Kateryna, Weissensteiner, Matthias, Cremona, Marzia, Guiblet, Wilfried, Stoler, Nicholas, Harris, Robert, and Cechova, Monika

Subjects

Humans, Nucleotide Motifs, DNA, Z-Form, Sequence Analysis, DNA, DNA, Base Composition, High-Throughput Nucleotide Sequencing, Nanopores

Abstract

Approximately 13% of the human genome at certain motifs have the potential to form noncanonical (non-B) DNA structures (e.g., G-quadruplexes, cruciforms, and Z-DNA), which regulate many cellular processes but also affect the activity of polymerases and helicases. Because sequencing technologies use these enzymes, they might possess increased errors at non-B structures. To evaluate this, we analyzed error rates, read depth, and base quality of Illumina, Pacific Biosciences (PacBio) HiFi, and Oxford Nanopore Technologies (ONT) sequencing at non-B motifs. All technologies showed altered sequencing success for most non-B motif types, although this could be owing to several factors, including structure formation, biased GC content, and the presence of homopolymers. Single-nucleotide mismatch errors had low biases in HiFi and ONT for all non-B motif types but were increased for G-quadruplexes and Z-DNA in all three technologies. Deletion errors were increased for all non-B types but Z-DNA in Illumina and HiFi, as well as only for G-quadruplexes in ONT. Insertion errors for non-B motifs were highly, moderately, and slightly elevated in Illumina, HiFi, and ONT, respectively. Additionally, we developed a probabilistic approach to determine the number of false positives at non-B motifs depending on sample size and variant frequency, and applied it to publicly available data sets (1000 Genomes, Simons Genome Diversity Project, and gnomAD). We conclude that elevated sequencing errors at non-B DNA motifs should be considered in low-read-depth studies (single-cell, ancient DNA, and pooled-sample population sequencing) and in scoring rare variants. Combining technologies should maximize sequencing accuracy in future studies of non-B DNA.

Published

2023

2. Performance of Cervical Screening a Decade Following HPV Vaccination: The Costa Rica Vaccine Trial.

Author

Hu, Shang-Ying, Kreimer, Aimée, Porras, Carolina, Guillén, Diego, Alfaro, Mario, Darragh, Teresa, Stoler, Mark, Villegas, Luis, Ocampo, Rebecca, Rodriguez, Ana, Schiffman, Mark, Tsang, Sabrina, Lowy, Douglas, Schiller, John, Schussler, John, Quint, Wim, Gail, Mitchell, Sampson, Joshua, Hildesheim, Allan, and Herrero, Rolando

Subjects

Costa Rica, Early Detection of Cancer, Female, Human papillomavirus 16, Human papillomavirus 18, Humans, Papillomaviridae, Papillomavirus Infections, Papillomavirus Vaccines, Uterine Cervical Neoplasms, Vaccination, Young Adult

Abstract

BACKGROUND: We investigated the impact of human papillomavirus (HPV) vaccination on the performance of cytology-based and HPV-based screening for detection of cervical precancer among women vaccinated as young adults and reaching screening age. METHODS: A total of 4632 women aged 25-36 years from the Costa Rica HPV Vaccine Trial were included (2418 HPV-vaccinated as young adults and 2214 unvaccinated). We assessed the performance of cytology- and HPV-based cervical screening modalities in vaccinated and unvaccinated women to detect high-grade cervical precancers diagnosed over 4 years and the absolute risk of cumulative cervical precancers by screening results at entry. RESULTS: We detected 95 cervical intraepithelial neoplasia grade 3 or worse (52 in unvaccinated and 43 in vaccinated women). HPV16/18/31/33/45 was predominant (69%) among unvaccinated participants, and HPV35/52/58/39/51/56/59/66/68 predominated (65%) among vaccinated participants. Sensitivity and specificity of cervical screening approaches were comparable between women vaccinated as young adults and unvaccinated women. Colposcopy referral rates were lower in the vaccinated group for HPV-based screening modalities, but the positive predictive value was comparable between the 2 groups. CONCLUSIONS: Among women approaching screening ages, vaccinated as young adults, and with a history of intensive screening, the expected reduction in the positive predictive value of HPV testing, associated with dropping prevalence of HPV-associated lesions, was not observed. This is likely due to the presence of high-grade lesions associated with nonvaccine HPV types, which may be less likely to progress to cancer.

Published

2022

3. A novel DPH5-related diphthamide-deficiency syndrome causing embryonic lethality or profound neurodevelopmental disorder

Author

Shankar, Suma P, Grimsrud, Kristin, Lanoue, Louise, Egense, Alena, Willis, Brandon, Hörberg, Johanna, AlAbdi, Mayer, Klaus, Ütkür, Koray, Monaghan, Kristin G, Krier, Joel, Stoler, Joan, Alnemer, Maha, Shankar, Prabhu R, Schaffrath, Raffael, Alkuraya, Fowzan S, Brinkmann, Ulrich, Eriksson, Leif A, Lloyd, Kent, Rauen, Katherine A, Network, Undiagnosed Diseases, Acosta, Maria T, Adam, Margaret, Adams, David R, Alvey, Justin, Amendola, Laura, Andrews, Ashley, Ashley, Euan A, Azamian, Mahshid S, Bacino, Carlos A, Bademci, Guney, Balasubramanyam, Ashok, Baldridge, Dustin, Bale, Jim, Bamshad, Michael, Barbouth, Deborah, Bayrak-Toydemir, Pinar, Beck, Anita, Beggs, Alan H, Behrens, Edward, Bejerano, Gill, Bennet, Jimmy, Berg-Rood, Beverly, Bernstein, Jonathan A, Berry, Gerard T, Bican, Anna, Bivona, Stephanie, Blue, Elizabeth, Bohnsack, John, Bonner, Devon, Botto, Lorenzo, Boyd, Brenna, Briere, Lauren C, Brokamp, Elly, Brown, Gabrielle, Burke, Elizabeth A, Burrage, Lindsay C, Butte, Manish J, Byers, Peter, Byrd, William E, Carey, John, Carrasquillo, Olveen, Cassini, Thomas, Chang, Ta Chen Peter, Chanprasert, Sirisak, Chao, Hsiao-Tuan, Clark, Gary D, Coakley, Terra R, Cobban, Laurel A, Cogan, Joy D, Coggins, Matthew, Cole, F Sessions, Colley, Heather A, Cooper, Cynthia M, Cope, Heidi, Craigen, William J, Crouse, Andrew B, Cunningham, Michael, D'Souza, Precilla, Dai, Hongzheng, Dasari, Surendra, Davis, Joie, Dayal, Jyoti G, Deardorff, Matthew, Dell'Angelica, Esteban C, Dipple, Katrina, Doherty, Daniel, Dorrani, Naghmeh, Doss, Argenia L, Douine, Emilie D, Duncan, Laura, Earl, Dawn, Eckstein, David J, Emrick, Lisa T, Eng, Christine M, Esteves, Cecilia, Falk, Marni, Fernandez, Liliana, Fieg, Elizabeth L, and Fisher, Paul G

Subjects

Biological Sciences, Bioinformatics and Computational Biology, Genetics, Pediatric, Human Genome, 2.1 Biological and endogenous factors, Adenosine Diphosphate, Animals, Histidine, Humans, Methyltransferases, Mice, Mice, Inbred C57BL, Neurodevelopmental Disorders, Saccharomyces cerevisiae, Saccharomyces cerevisiae Proteins, Syndrome, Nonverbal neurodevelopment delays, Novel gene discovery, Precision animal modeling, Precision genomics, Translational genetics, Undiagnosed Diseases Network, Clinical Sciences, Genetics & Heredity

Abstract

PurposeDiphthamide is a post-translationally modified histidine essential for messenger RNA translation and ribosomal protein synthesis. We present evidence for DPH5 as a novel cause of embryonic lethality and profound neurodevelopmental delays (NDDs).MethodsMolecular testing was performed using exome or genome sequencing. A targeted Dph5 knockin mouse (C57BL/6Ncrl-Dph5em1Mbp/Mmucd) was created for a DPH5 p.His260Arg homozygous variant identified in 1 family. Adenosine diphosphate-ribosylation assays in DPH5-knockout human and yeast cells and in silico modeling were performed for the identified DPH5 potential pathogenic variants.ResultsDPH5 variants p.His260Arg (homozygous), p.Asn110Ser and p.Arg207Ter (heterozygous), and p.Asn174LysfsTer10 (homozygous) were identified in 3 unrelated families with distinct overlapping craniofacial features, profound NDDs, multisystem abnormalities, and miscarriages. Dph5 p.His260Arg homozygous knockin was embryonically lethal with only 1 subviable mouse exhibiting impaired growth, craniofacial dysmorphology, and multisystem dysfunction recapitulating the human phenotype. Adenosine diphosphate-ribosylation assays showed absent to decreased function in DPH5-knockout human and yeast cells. In silico modeling of the variants showed altered DPH5 structure and disruption of its interaction with eEF2.ConclusionWe provide strong clinical, biochemical, and functional evidence for DPH5 as a novel cause of embryonic lethality or profound NDDs with multisystem involvement and expand diphthamide-deficiency syndromes and ribosomopathies.

Published

2022

4. Heterozygous loss-of-function variants significantly expand the phenotypes associated with loss of GDF11

Author

Ravenscroft, Thomas A, Phillips, Jennifer B, Fieg, Elizabeth, Bajikar, Sameer S, Peirce, Judy, Wegner, Jeremy, Luna, Alia A, Fox, Eric J, Yan, Yi-Lin, Rosenfeld, Jill A, Zirin, Jonathan, Kanca, Oguz, Benke, Paul J, Cameron, Eric S, Strehlow, Vincent, Platzer, Konrad, Jamra, Rami Abou, Klöckner, Chiara, Osmond, Matthew, Licata, Thomas, Rojas, Samantha, Dyment, David, Chong, Josephine SC, Lincoln, Sharyn, Stoler, Joan M, Postlethwait, John H, Wangler, Michael F, Yamamoto, Shinya, Krier, Joel, Westerfield, Monte, and Bellen, Hugo J

Subjects

Congenital Structural Anomalies, Genetics, Pediatric, 2.1 Biological and endogenous factors, Detection, screening and diagnosis, 4.1 Discovery and preclinical testing of markers and technologies, Aetiology, Animals, Bone Morphogenetic Proteins, Craniofacial Abnormalities, Growth Differentiation Factors, Humans, Mutation, Missense, Phenotype, Spine, Zebrafish, Undiagnosed Diseases Network, Clinical Sciences, Genetics & Heredity

Abstract

PurposeGrowth differentiation factor 11 (GDF11) is a key signaling protein required for proper development of many organ systems. Only one prior study has associated an inherited GDF11 variant with a dominant human disease in a family with variable craniofacial and vertebral abnormalities. Here, we expand the phenotypic spectrum associated with GDF11 variants and document the nature of the variants.MethodsWe present a cohort of six probands with de novo and inherited nonsense/frameshift (4/6 patients) and missense (2/6) variants in GDF11. We generated gdf11 mutant zebrafish to model loss of gdf11 phenotypes and used an overexpression screen in Drosophila to test variant functionality.ResultsPatients with variants in GDF11 presented with craniofacial (5/6), vertebral (5/6), neurological (6/6), visual (4/6), cardiac (3/6), auditory (3/6), and connective tissue abnormalities (3/6). gdf11 mutant zebrafish show craniofacial abnormalities and body segmentation defects that match some patient phenotypes. Expression of the patients' variants in the fly showed that one nonsense variant in GDF11 is a severe loss-of-function (LOF) allele whereas the missense variants in our cohort are partial LOF variants.ConclusionGDF11 is needed for human development, particularly neuronal development, and LOF GDF11 alleles can affect the development of numerous organs and tissues.

Published

2021

5. Risk Factors for Non–Human Papillomavirus (HPV) Type 16/18 Cervical Infections and Associated Lesions Among HPV DNA–Negative Women Vaccinated Against HPV-16/18 in the Costa Rica Vaccine Trial

Author

Sierra, Mónica S, Tsang, Sabrina H, Hu, Shangying, Porras, Carolina, Herrero, Rolando, Kreimer, Aimée R, Schussler, John, Boland, Joseph, Wagner, Sarah, Cortes, Bernal, Rodríguez, Ana C, Quint, Wim, van Doorn, Leen-Jan, Schiffman, Mark, Sampson, Joshua N, Hildesheim, Allan, Cortés, Bernal, González, Paula, Jiménez, Silvia E, Rodríguez, Ana Cecilia, Lowy, Douglas R, Schiller, John T, Sherman, Mark, Wacholder, Sholom, Pinto, Ligia A, Kemp, Troy J, Sidawy, Mary K, Struijk, Linda, Palefsky, Joel M, Darragh, Teresa M, and Stoler, Mark H

Subjects

Clinical Research, Behavioral and Social Science, Clinical Trials and Supportive Activities, Sexually Transmitted Infections, HPV and/or Cervical Cancer Vaccines, Immunization, Prevention, HIV/AIDS, Cervical Cancer, Adolescent Sexual Activity, Infectious Diseases, Vaccine Related, Pediatric, Cancer, Adolescent, Adult, Cervical Intraepithelial Neoplasia, Costa Rica, DNA, Female, Human papillomavirus 16, Human papillomavirus 18, Humans, Papillomaviridae, Papillomavirus Infections, Papillomavirus Vaccines, Pregnancy, Risk Factors, Treatment Outcome, Uterine Cervical Neoplasms, Young Adult, Costa Rica Human Papillomavirus Vaccine Trial (CVT) Group, Uterine Cervical Dysplasia, CIN2+, HPV infection, HPV vaccine, incidence, persistence, progression, Biological Sciences, Medical and Health Sciences, Microbiology

Abstract

BackgroundFactors that lead human papillomavirus (HPV) infections to persist and progress to cancer are not fully understood. We evaluated co-factors for acquisition, persistence, and progression of non-HPV-16/18 infections among HPV-vaccinated women.MethodsWe analyzed 2153 women aged 18-25 years randomized to the HPV-vaccine arm of the Costa Rica HPV Vaccine Trial. Women were HPV DNA negative for all types at baseline and followed for approximately 11 years. Generalized estimating equation methods were used to account for correlated observations. Time-dependent factors evaluated were age, sexual behavior, marital status, hormonally related factors, number of full-term pregnancies (FTPs), smoking behavior, and baseline body mass index.ResultsA total of 1777 incident oncogenic non-HPV-16/18 infections were detected in 12 292 visits (average, 0.14 infections/visit). Age and sexual behavior-related variables were associated with oncogenic non-HPV-16/18 acquisition. Twenty-six percent of incident infections persisted for ≥1 year. None of the factors evaluated were statistically associated with persistence of oncogenic non-HPV-16/18 infections. Risk of progression to Cervical Intraepithelial Neoplasia grade 2 or worst (CIN2+) increased with increasing age (P for trend = .001), injectable contraceptive use (relative risk, 2.61 [95% confidence interval, 1.19-5.73] ever vs never), and increasing FTPs (P for trend = .034).ConclusionsIn a cohort of HPV-16/18-vaccinated women, age and sexual behavior variables are associated with acquisition of oncogenic non-HPV-16/18 infections; no notable factors are associated with persistence of acquired infections; and age, parity, and hormonally related exposures are associated with progression to CIN2+.

Published

2021

6. Expanding the genotypic and phenotypic spectrum in a diverse cohort of 104 individuals with Wiedemann‐Steiner syndrome

Author

Sheppard, Sarah E, Campbell, Ian M, Harr, Margaret H, Gold, Nina, Li, Dong, Bjornsson, Hans T, Cohen, Julie S, Fahrner, Jill A, Fatemi, Ali, Harris, Jacqueline R, Nowak, Catherine, Stevens, Cathy A, Grand, Katheryn, Au, Margaret, Graham, John M, Sanchez‐Lara, Pedro A, Del Campo, Miguel, Jones, Marilyn C, Abdul‐Rahman, Omar, Alkuraya, Fowzan S, Bassetti, Jennifer A, Bergstrom, Katherine, Bhoj, Elizabeth, Dugan, Sarah, Kaplan, Julie D, Derar, Nada, Gripp, Karen W, Hauser, Natalie, Innes, A Micheil, Keena, Beth, Kodra, Neslida, Miller, Rebecca, Nelson, Beverly, Nowaczyk, Malgorzata J, Rahbeeni, Zuhair, Ben‐Shachar, Shay, Shieh, Joseph T, Slavotinek, Anne, Sobering, Andrew K, Abbott, Mary‐Alice, Allain, Dawn C, Amlie‐Wolf, Louise, Au, Ping Yee Billie, Bedoukian, Emma, Beek, Geoffrey, Barry, James, Berg, Janet, Bernstein, Jonathan A, Cytrynbaum, Cheryl, Chung, Brian Hon‐Yin, Donoghue, Sarah, Dorrani, Naghmeh, Eaton, Alison, Flores‐Daboub, Josue A, Dubbs, Holly, Felix, Carolyn A, Fong, Chin‐To, Fung, Jasmine Lee Fong, Gangaram, Balram, Goldstein, Amy, Greenberg, Rotem, Ha, Thoa K, Hersh, Joseph, Izumi, Kosuke, Kallish, Staci, Kravets, Elijah, Kwok, Pui‐Yan, Jobling, Rebekah K, Johnson, Amy E Knight, Kushner, Jessica, Lee, Bo Hoon, Levin, Brooke, Lindstrom, Kristin, Manickam, Kandamurugu, Mardach, Rebecca, McCormick, Elizabeth, McLeod, D Ross, Mentch, Frank D, Minks, Kelly, Muraresku, Colleen, Nelson, Stanley F, Porazzi, Patrizia, Pichurin, Pavel N, Powell‐Hamilton, Nina N, Powis, Zoe, Ritter, Alyssa, Rogers, Caleb, Rohena, Luis, Ronspies, Carey, Schroeder, Audrey, Stark, Zornitza, Starr, Lois, Stoler, Joan, Suwannarat, Pim, Velinov, Milen, Weksberg, Rosanna, Wilnai, Yael, Zadeh, Neda, Zand, Dina J, and Falk, Marni J

Subjects

Congenital Structural Anomalies, Clinical Research, Brain Disorders, Rare Diseases, Pediatric, Aetiology, 2.1 Biological and endogenous factors, Black People, Constipation, Failure to Thrive, Genetic Association Studies, Genetic Predisposition to Disease, Growth Disorders, Histone-Lysine N-Methyltransferase, Humans, Hypertrichosis, Intellectual Disability, Loss of Function Mutation, Myeloid-Lymphoid Leukemia Protein, Retrospective Studies, White People, hypertrichosis, KMT2A, MLL1, syndromic intellectual disability, syndromic short stature, Wiedemann&#8208, Steiner syndrome, Wiedemann-Steiner syndrome, Genetics, Clinical Sciences

Abstract

Wiedemann-Steiner syndrome (WSS) is an autosomal dominant disorder caused by monoallelic variants in KMT2A and characterized by intellectual disability and hypertrichosis. We performed a retrospective, multicenter, observational study of 104 individuals with WSS from five continents to characterize the clinical and molecular spectrum of WSS in diverse populations, to identify physical features that may be more prevalent in White versus Black Indigenous People of Color individuals, to delineate genotype-phenotype correlations, to define developmental milestones, to describe the syndrome through adulthood, and to examine clinicians' differential diagnoses. Sixty-nine of the 82 variants (84%) observed in the study were not previously reported in the literature. Common clinical features identified in the cohort included: developmental delay or intellectual disability (97%), constipation (63.8%), failure to thrive (67.7%), feeding difficulties (66.3%), hypertrichosis cubiti (57%), short stature (57.8%), and vertebral anomalies (46.9%). The median ages at walking and first words were 20 months and 18 months, respectively. Hypotonia was associated with loss of function (LoF) variants, and seizures were associated with non-LoF variants. This study identifies genotype-phenotype correlations as well as race-facial feature associations in an ethnically diverse cohort, and accurately defines developmental trajectories, medical comorbidities, and long-term outcomes in individuals with WSS.

Published

2021

7. Efficacy of the bivalent HPV vaccine against HPV 16/18-associated precancer: long-term follow-up results from the Costa Rica Vaccine Trial.

Author

Porras, Carolina, Tsang, Sabrina H, Herrero, Rolando, Guillén, Diego, Darragh, Teresa M, Stoler, Mark H, Hildesheim, Allan, Wagner, Sarah, Boland, Joseph, Lowy, Douglas R, Schiller, John T, Schiffman, Mark, Schussler, John, Gail, Mitchell H, Quint, Wim, Ocampo, Rebeca, Morales, Jorge, Rodríguez, Ana C, Hu, Shangying, Sampson, Joshua N, Kreimer, Aimée R, and Costa Rica Vaccine Trial Group

Subjects

Costa Rica Vaccine Trial Group, Humans, Papillomavirus Infections, Vaccines, Combined, Treatment Outcome, Immunization, Double-Blind Method, Time Factors, Adolescent, Adult, Costa Rica, Uterine Cervical Dysplasia, Uterine Cervical Neoplasms, Female, Human papillomavirus 18, Human papillomavirus 16, Papillomavirus Vaccines, Young Adult, Neoplasm Grading, Cervical Cancer, Vaccine Related, Cancer, Biotechnology, HPV and/or Cervical Cancer Vaccines, Clinical Trials and Supportive Activities, Prevention, Clinical Research, HIV/AIDS, Sexually Transmitted Infections, Infectious Diseases, 3.4 Vaccines, Prevention of disease and conditions, and promotion of well-being, Infection, Good Health and Well Being, Oncology and Carcinogenesis, Oncology & Carcinogenesis

Abstract

BackgroundOncogenic human papillomavirus (HPV) infections cause most cases of cervical cancer. Here, we report long-term follow-up results for the Costa Rica Vaccine Trial (publicly funded and initiated before licensure of the HPV vaccines), with the aim of assessing the efficacy of the bivalent HPV vaccine for preventing HPV 16/18-associated cervical intraepithelial neoplasia grade 2 or worse (CIN2+).MethodsWomen aged 18-25 years were enrolled in a randomised, double-blind, controlled trial in Costa Rica, between June 28, 2004, and Dec 21, 2005, designed to assess the efficacy of a bivalent vaccine for the prevention of infection with HPV 16/18 and associated precancerous lesions at the cervix. Participants were randomly assigned (1:1) to receive an HPV 16/18 AS04-adjuvanted vaccine or control hepatitis A vaccine. Vaccines were administered intramuscularly in three 0·5 mL doses at 0, 1, and 6 months and participants were followed up annually for 4 years. After the blinded phase, women in the HPV vaccine group were invited to enrol in the long-term follow-up study, which extended follow-up for 7 additional years. The control group received HPV vaccine and was replaced with a new unvaccinated control group. Women were followed up every 2 years until year 11. Investigators and patients were aware of treatment allocation for the follow-up phase. At each visit, clinicians collected cervical cells from sexually active women for cytology and HPV testing. Women with abnormal cytology were referred to colposcopy, biopsy, and treatment as needed. Women with negative results at the last screening visit (year 11) exited the long-term follow-up study. The analytical cohort for vaccine efficacy included women who were HPV 16/18 DNA-negative at vaccination. The primary outcome of this analysis was defined as histopathologically confirmed CIN2+ or cervical intraepithelial neoplasia grade 3 or worse associated with HPV 16/18 cervical infection detected at colposcopy referral. We calculated vaccine efficacy by year and cumulatively. This long-term follow-up study is registered with ClinicalTrials.gov, NCT00867464.Findings7466 women were enrolled in the Costa Rica Vaccine Trial; 3727 received the HPV vaccine and 3739 received the control vaccine. Between March 30, 2009, and July 5, 2012, 2635 women in the HPV vaccine group and 2836 women in the new unvaccinated control group were enrolled in the long-term follow-up study. 2635 women in the HPV vaccine group and 2677 women in the control group were included in the analysis cohort for years 0-4, and 2073 women from the HPV vaccine group and 2530 women from the new unvaccinated control group were included in the analysis cohort for years 7-11. Median follow-up time for the HPV group was 11·1 years (IQR 9·1-11·7), 4·6 years (4·3-5·3) for the original control group, and 6·2 years (5·5-6·9) for the new unvaccinated control group. At year 11, vaccine efficacy against incident HPV 16/18-associated CIN2+ was 100% (95% CI 89·2-100·0); 34 (1·5%) of 2233 unvaccinated women had a CIN2+ outcome compared with none of 1913 women in the HPV group. Cumulative vaccine efficacy against HPV 16/18-associated CIN2+ over the 11-year period was 97·4% (95% CI 88·0-99·6). Similar protection was observed against HPV 16/18-associated CIN3-specifically at year 11, vaccine efficacy was 100% (95% CI 78·8-100·0) and cumulative vaccine efficacy was 94·9% (73·7-99·4). During the long-term follow-up, no serious adverse events occurred that were deemed related to the HPV vaccine. The most common grade 3 or worse serious adverse events were pregnancy, puerperium, and perinatal conditions (in 255 [10%] of 2530 women in the unvaccinated control group and 201 [10%] of 2073 women in the HPV vaccine group). Four women in the unvaccinated control group and three in the HPV vaccine group died; no deaths were deemed to be related to the HPV vaccine.InterpretationThe bivalent HPV vaccine has high efficacy against HPV 16/18-associated precancer for more than a decade after initial vaccination, supporting the notion that invasive cervical cancer is preventable.FundingUS National Cancer Institute.

Published

2020

8. Efficacy of the bivalent HPV vaccine against HPV 16/18-associated precancer: long-term follow-up results from the Costa Rica Vaccine Trial.

Author

Porras, Carolina, Tsang, Sabrina H, Herrero, Rolando, Guillén, Diego, Darragh, Teresa M, Stoler, Mark H, Hildesheim, Allan, Wagner, Sarah, Boland, Joseph, Lowy, Douglas R, Schiller, John T, Schiffman, Mark, Schussler, John, Gail, Mitchell H, Quint, Wim, Ocampo, Rebeca, Morales, Jorge, Rodríguez, Ana C, Hu, Shangying, Sampson, Joshua N, Kreimer, Aimée R, and Costa Rica Vaccine Trial Group

Subjects

Costa Rica Vaccine Trial Group, Humans, Papillomavirus Infections, Cervical Intraepithelial Neoplasia, Vaccines, Combined, Treatment Outcome, Immunization, Double-Blind Method, Time Factors, Adolescent, Adult, Costa Rica, Uterine Cervical Neoplasms, Female, Human papillomavirus 18, Human papillomavirus 16, Papillomavirus Vaccines, Young Adult, Neoplasm Grading, Vaccines, Combined, Oncology & Carcinogenesis, Oncology and Carcinogenesis

Abstract

BackgroundOncogenic human papillomavirus (HPV) infections cause most cases of cervical cancer. Here, we report long-term follow-up results for the Costa Rica Vaccine Trial (publicly funded and initiated before licensure of the HPV vaccines), with the aim of assessing the efficacy of the bivalent HPV vaccine for preventing HPV 16/18-associated cervical intraepithelial neoplasia grade 2 or worse (CIN2+).MethodsWomen aged 18-25 years were enrolled in a randomised, double-blind, controlled trial in Costa Rica, between June 28, 2004, and Dec 21, 2005, designed to assess the efficacy of a bivalent vaccine for the prevention of infection with HPV 16/18 and associated precancerous lesions at the cervix. Participants were randomly assigned (1:1) to receive an HPV 16/18 AS04-adjuvanted vaccine or control hepatitis A vaccine. Vaccines were administered intramuscularly in three 0·5 mL doses at 0, 1, and 6 months and participants were followed up annually for 4 years. After the blinded phase, women in the HPV vaccine group were invited to enrol in the long-term follow-up study, which extended follow-up for 7 additional years. The control group received HPV vaccine and was replaced with a new unvaccinated control group. Women were followed up every 2 years until year 11. Investigators and patients were aware of treatment allocation for the follow-up phase. At each visit, clinicians collected cervical cells from sexually active women for cytology and HPV testing. Women with abnormal cytology were referred to colposcopy, biopsy, and treatment as needed. Women with negative results at the last screening visit (year 11) exited the long-term follow-up study. The analytical cohort for vaccine efficacy included women who were HPV 16/18 DNA-negative at vaccination. The primary outcome of this analysis was defined as histopathologically confirmed CIN2+ or cervical intraepithelial neoplasia grade 3 or worse associated with HPV 16/18 cervical infection detected at colposcopy referral. We calculated vaccine efficacy by year and cumulatively. This long-term follow-up study is registered with ClinicalTrials.gov, NCT00867464.Findings7466 women were enrolled in the Costa Rica Vaccine Trial; 3727 received the HPV vaccine and 3739 received the control vaccine. Between March 30, 2009, and July 5, 2012, 2635 women in the HPV vaccine group and 2836 women in the new unvaccinated control group were enrolled in the long-term follow-up study. 2635 women in the HPV vaccine group and 2677 women in the control group were included in the analysis cohort for years 0-4, and 2073 women from the HPV vaccine group and 2530 women from the new unvaccinated control group were included in the analysis cohort for years 7-11. Median follow-up time for the HPV group was 11·1 years (IQR 9·1-11·7), 4·6 years (4·3-5·3) for the original control group, and 6·2 years (5·5-6·9) for the new unvaccinated control group. At year 11, vaccine efficacy against incident HPV 16/18-associated CIN2+ was 100% (95% CI 89·2-100·0); 34 (1·5%) of 2233 unvaccinated women had a CIN2+ outcome compared with none of 1913 women in the HPV group. Cumulative vaccine efficacy against HPV 16/18-associated CIN2+ over the 11-year period was 97·4% (95% CI 88·0-99·6). Similar protection was observed against HPV 16/18-associated CIN3-specifically at year 11, vaccine efficacy was 100% (95% CI 78·8-100·0) and cumulative vaccine efficacy was 94·9% (73·7-99·4). During the long-term follow-up, no serious adverse events occurred that were deemed related to the HPV vaccine. The most common grade 3 or worse serious adverse events were pregnancy, puerperium, and perinatal conditions (in 255 [10%] of 2530 women in the unvaccinated control group and 201 [10%] of 2073 women in the HPV vaccine group). Four women in the unvaccinated control group and three in the HPV vaccine group died; no deaths were deemed to be related to the HPV vaccine.InterpretationThe bivalent HPV vaccine has high efficacy against HPV 16/18-associated precancer for more than a decade after initial vaccination, supporting the notion that invasive cervical cancer is preventable.FundingUS National Cancer Institute.

Published

2020

9. Analysis of Ugandan cervical carcinomas identifies human papillomavirus clade-specific epigenome and transcriptome landscapes.

Author

Gagliardi, Alessia, Porter, Vanessa L, Zong, Zusheng, Bowlby, Reanne, Titmuss, Emma, Namirembe, Constance, Griner, Nicholas B, Petrello, Hilary, Bowen, Jay, Chan, Simon K, Culibrk, Luka, Darragh, Teresa M, Stoler, Mark H, Wright, Thomas C, Gesuwan, Patee, Dyer, Maureen A, Ma, Yussanne, Mungall, Karen L, Jones, Steven JM, Nakisige, Carolyn, Novik, Karen, Orem, Jackson, Origa, Martin, Gastier-Foster, Julie M, Yarchoan, Robert, Casper, Corey, Mills, Gordon B, Rader, Janet S, Ojesina, Akinyemi I, Gerhard, Daniela S, Mungall, Andrew J, and Marra, Marco A

Subjects

Humans, Papillomaviridae, Papillomavirus Infections, Signal Transduction, DNA Methylation, Up-Regulation, Adult, Aged, Middle Aged, Uganda, Uterine Cervical Neoplasms, Female, Promoter Regions, Genetic, Transcriptome, Epigenome, Promoter Regions, Genetic, Developmental Biology, Biological Sciences, Medical and Health Sciences

Abstract

Cervical cancer is the most common cancer affecting sub-Saharan African women and is prevalent among HIV-positive (HIV+) individuals. No comprehensive profiling of cancer genomes, transcriptomes or epigenomes has been performed in this population thus far. We characterized 118 tumors from Ugandan patients, of whom 72 were HIV+, and performed extended mutation analysis on an additional 89 tumors. We detected human papillomavirus (HPV)-clade-specific differences in tumor DNA methylation, promoter- and enhancer-associated histone marks, gene expression and pathway dysregulation. Changes in histone modification at HPV integration events were correlated with upregulation of nearby genes and endogenous retroviruses.

Published

2020

10. Efficacy of the AS04-adjuvanted HPV-16/18 vaccine: Pooled analysis of the Costa Rica Vaccine and PATRICIA randomized controlled trials

Author

Tota, Joseph E, Struyf, Frank, Sampson, Joshua N, Gonzalez, Paula, Ryser, Martin, Herrero, Rolando, Schussler, John, Karkada, Naveen, Rodriguez, Ana Cecilia, Folschweiller, Nicolas, Porras, Carolina, Schiffman, Mark, Schiller, John T, Quint, Wim, Kreimer, Aimée R, Wheeler, Cosette M, Hildesheim, Allan, Cortés, Bernal, González, Paula, Jiménez, Silvia E, Rodríguez, Ana Cecilia, Lowy, Douglas R, Wacholder, Sholom, Pinto, Ligia A, Kemp, Troy J, van Doorn, Leen-Jan, Struijk, Linda, Palefsky, Joel M, Darragh, Teresa M, Stoler, Mark H, Garland, SM, Skinner, SR, De Sutter, P, Poppe, WAJ, De Carvalho, NS, Teixeira, JC, Ferguson, L, Ferguson, M, Papp, K, Ramjattan, B, Orr, PH, Paavonen, J, Höpker, WD, Tobgui, S Jensen-El, Liverani, CA, Limson, GM, Marti, M Campins, Castro, M, Centeno, C, Chow, SN, Angsuwathana, S, Lewis, D, Ackerman, R, Caldwell, M, Chambers, C, Chatterjee, A, Harper, D, Sperling, R, Stapleton, J, Waldbaum, A, Lee, P, and Awedikian, Rafi

Subjects

Sexually Transmitted Infections, Immunization, Cancer, Biotechnology, Infectious Diseases, HPV and/or Cervical Cancer Vaccines, Vaccine Related, Clinical Research, Clinical Trials and Supportive Activities, Cervical Cancer, Prevention, HIV/AIDS, Adjuvants, Immunologic, Adolescent, Adult, Costa Rica, Female, Human papillomavirus 16, Human papillomavirus 18, Humans, Papillomavirus Infections, Papillomavirus Vaccines, Randomized Controlled Trials as Topic, Retrospective Studies, Treatment Outcome, Uterine Cervical Neoplasms, Young Adult, Uterine Cervical Dysplasia, Costa Rica Vaccine Trial and PATRICIA Study, Oncology and Carcinogenesis, Oncology & Carcinogenesis

Abstract

BackgroundThe AS04-adjuvanted HPV16/18 (AS04-HPV16/18) vaccine provides excellent protection against targeted human papillomavirus (HPV) types and a variable degree of cross-protection against others, including types 6/11/31/33/45. High efficacy against any cervical intraepithelial neoplasia grade 3 or greater (CIN3+; >90%) suggests that lower levels of protection may exist for a wide range of oncogenic HPV types, which is difficult to quantify in individual trials. Pooling individual-level data from two randomized controlled trials, we aimed to evaluate AS04-HPV16/18 vaccine efficacy against incident HPV infections and cervical abnormalities .MethodsData were available from the Costa Rica Vaccine Trial (NCT00128661) and Papilloma Trial Against Cancer in Young Adults trial (NCT00122681), two large-scale, double-blind randomized controlled trials of the AS04-HPV16/18 vaccine. Primary analyses focused on disease-free women with no detectable cervicovaginal HPV at baseline.ResultsA total of 12 550 women were included in our primary analyses (HPV arm = 6271, control arm = 6279). Incidence of 6-month persistent oncogenic and nononcogenic infections, excluding known and accepted protected types 6/11/16/18/31/33/45 (focusing on 34/35/39/40/42/43/44/51/52/53/54/56/58/59/66/68/73/70/74), was statistically significantly lower in the HPV arm than in the control arm (efficacy = 9.9%, 95% confidence interval [CI] = 1.7% to 17.4%). Statistically significant efficacy (P

Published

2020

11. Analysis of Ugandan cervical carcinomas identifies human papillomavirus clade-specific epigenome and transcriptome landscapes.

Author

Gagliardi, Alessia, Porter, Vanessa L, Zong, Zusheng, Bowlby, Reanne, Titmuss, Emma, Namirembe, Constance, Griner, Nicholas B, Petrello, Hilary, Bowen, Jay, Chan, Simon K, Culibrk, Luka, Darragh, Teresa M, Stoler, Mark H, Wright, Thomas C, Gesuwan, Patee, Dyer, Maureen A, Ma, Yussanne, Mungall, Karen L, Jones, Steven JM, Nakisige, Carolyn, Novik, Karen, Orem, Jackson, Origa, Martin, Gastier-Foster, Julie M, Yarchoan, Robert, Casper, Corey, Mills, Gordon B, Rader, Janet S, Ojesina, Akinyemi I, Gerhard, Daniela S, Mungall, Andrew J, and Marra, Marco A

Subjects

Humans, Papillomaviridae, Papillomavirus Infections, Signal Transduction, DNA Methylation, Up-Regulation, Adult, Aged, Middle Aged, Uganda, Uterine Cervical Neoplasms, Female, Promoter Regions, Genetic, Transcriptome, Epigenome, Sexually Transmitted Infections, Cancer, Genetics, Cervical Cancer, Human Genome, HIV/AIDS, Infectious Diseases, Clinical Research, 2.1 Biological and endogenous factors, Aetiology, Infection, Biological Sciences, Medical and Health Sciences, Developmental Biology

Abstract

Cervical cancer is the most common cancer affecting sub-Saharan African women and is prevalent among HIV-positive (HIV+) individuals. No comprehensive profiling of cancer genomes, transcriptomes or epigenomes has been performed in this population thus far. We characterized 118 tumors from Ugandan patients, of whom 72 were HIV+, and performed extended mutation analysis on an additional 89 tumors. We detected human papillomavirus (HPV)-clade-specific differences in tumor DNA methylation, promoter- and enhancer-associated histone marks, gene expression and pathway dysregulation. Changes in histone modification at HPV integration events were correlated with upregulation of nearby genes and endogenous retroviruses.

Published

2020

12. Relationships of p16 Immunohistochemistry and Other Biomarkers With Diagnoses of Cervical Abnormalities: Implications for LAST Terminology

Author

Castle, Philip E, Adcock, Rachael, Cuzick, Jack, Wentzensen, Nicolas, Torrez-Martinez, Norah E, Torres, Salina M, Stoler, Mark H, Ronnett, Brigitte M, Joste, Nancy E, Darragh, Teresa M, Gravitt, Patti E, Schiffman, Mark, Hunt, William C, Kinney, Walter K, Wheeler, Cosette M, Committee, New Mexico HPV Pap Registry Steering, and Panel, p16 IHC Study

Subjects

Reproductive Medicine, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cervical Cancer, Infectious Diseases, Clinical Research, Cancer, Sexually Transmitted Infections, 4.2 Evaluation of markers and technologies, Detection, screening and diagnosis, Adult, Biomarkers, Tumor, Cyclin-Dependent Kinase Inhibitor p16, Female, Humans, Immunohistochemistry, Middle Aged, Papillomavirus Infections, Uterine Cervical Neoplasms, Uterine Cervical Dysplasia, New Mexico HPV Pap Registry Steering Committee, p16 IHC Study Panel, Clinical Sciences, Pathology, Clinical sciences

Abstract

Context.—Lower Anogenital Squamous Terminology (LAST) standardization recommended p16INK4a immunohistochemistry (p16 IHC) for biopsies diagnosed morphologically as cervical intraepithelial neoplasia (CIN) grade 2 (CIN2) to classify them as low-grade or high-grade squamous intraepithelial lesions (HSILs).Objective.—To describe the relationships of p16 IHC and other biomarkers associated with cervical cancer risk with biopsy diagnoses.Design.—A statewide, stratified sample of cervical biopsies diagnosed by community pathologists (CPs), including 1512 CIN2, underwent a consensus, expert pathologist panel (EP) review (without p16 IHC results), p16 IHC interpretation by a third pathology group, and human papillomavirus (HPV) genotyping, results of which were grouped hierarchically according to cancer risk. Antecedent cytologic interpretations were also available.Results.—Biopsies were more likely to test p16 IHC positive with increasing severity of CP diagnoses, overall (Ptrend ≤ .001) and within each HPV risk group (Ptrend ≤ .001 except for low-risk HPV [Ptrend < .010]). All abnormal grades of CP-diagnosed biopsies were more likely to test p16 IHC positive with a higher HPV risk group (Ptrend < .001), and testing p16 IHC positive was associated with higher HPV risk group than testing p16 IHC negative for each grade of CP-diagnosed biopsies (P < .001). p16 IHC-positive, CP-diagnosed CIN2 biopsies were less likely than CP-diagnosed CIN3 biopsies to test HPV16 positive, have an antecedent HSIL+ cytology, or to be diagnosed as CIN3+ by the EP (P < .001 for all). p16 IHC-positive, CP-diagnosed CIN1 biopsies had lower HPV risk groups than p16 IHC-negative, CP-diagnosed CIN2 biopsies (P < .001).Conclusions.—p16 IHC-positive, CP-diagnosed CIN2 appears to be lower cancer risk than CP-diagnosed CIN3. LAST classification of "HSIL" diagnosis, which includes p16 IHC-positive CIN2, should annotate the morphologic diagnosis (CIN2 or CIN3) to inform all management decisions, which is especially important for young (

Published

2020

13. Relationships of p16 Immunohistochemistry and Other Biomarkers With Diagnoses of Cervical Abnormalities: Implications for LAST Terminology.

Author

Gravitt, Patti, Schiffman, Mark, Hunt, William, Kinney, Walter, Wheeler, Cosette, Castle, Philip, Adcock, Rachael, Cuzick, Jack, Wentzensen, Nicolas, Torrez-Martinez, Norah, Torres, Salina, Stoler, Mark, Ronnett, Brigitte, Joste, Nancy, and Darragh, Teresa

Subjects

Adult, Biomarkers, Tumor, Cyclin-Dependent Kinase Inhibitor p16, Female, Humans, Immunohistochemistry, Middle Aged, Papillomavirus Infections, Uterine Cervical Neoplasms, Uterine Cervical Dysplasia

Abstract

CONTEXT.—: Lower Anogenital Squamous Terminology (LAST) standardization recommended p16INK4a immunohistochemistry (p16 IHC) for biopsies diagnosed morphologically as cervical intraepithelial neoplasia (CIN) grade 2 (CIN2) to classify them as low-grade or high-grade squamous intraepithelial lesions (HSILs). OBJECTIVE.—: To describe the relationships of p16 IHC and other biomarkers associated with cervical cancer risk with biopsy diagnoses. DESIGN.—: A statewide, stratified sample of cervical biopsies diagnosed by community pathologists (CPs), including 1512 CIN2, underwent a consensus, expert pathologist panel (EP) review (without p16 IHC results), p16 IHC interpretation by a third pathology group, and human papillomavirus (HPV) genotyping, results of which were grouped hierarchically according to cancer risk. Antecedent cytologic interpretations were also available. RESULTS.—: Biopsies were more likely to test p16 IHC positive with increasing severity of CP diagnoses, overall (Ptrend ≤ .001) and within each HPV risk group (Ptrend ≤ .001 except for low-risk HPV [Ptrend < .010]). All abnormal grades of CP-diagnosed biopsies were more likely to test p16 IHC positive with a higher HPV risk group (Ptrend < .001), and testing p16 IHC positive was associated with higher HPV risk group than testing p16 IHC negative for each grade of CP-diagnosed biopsies (P < .001). p16 IHC-positive, CP-diagnosed CIN2 biopsies were less likely than CP-diagnosed CIN3 biopsies to test HPV16 positive, have an antecedent HSIL+ cytology, or to be diagnosed as CIN3+ by the EP (P < .001 for all). p16 IHC-positive, CP-diagnosed CIN1 biopsies had lower HPV risk groups than p16 IHC-negative, CP-diagnosed CIN2 biopsies (P < .001). CONCLUSIONS.—: p16 IHC-positive, CP-diagnosed CIN2 appears to be lower cancer risk than CP-diagnosed CIN3. LAST classification of HSIL diagnosis, which includes p16 IHC-positive CIN2, should annotate the morphologic diagnosis (CIN2 or CIN3) to inform all management decisions, which is especially important for young (

Published

2020

14. Relationships of p16 Immunohistochemistry and Other Biomarkers With Diagnoses of Cervical Abnormalities: Implications for LAST Terminology.

Author

Castle, Philip E, Adcock, Rachael, Cuzick, Jack, Wentzensen, Nicolas, Torrez-Martinez, Norah E, Torres, Salina M, Stoler, Mark H, Ronnett, Brigitte M, Joste, Nancy E, Darragh, Teresa M, Gravitt, Patti E, Schiffman, Mark, Hunt, William C, Kinney, Walter K, Wheeler, Cosette M, New Mexico HPV Pap Registry Steering Committee, and p16 IHC Study Panel

Subjects

New Mexico HPV Pap Registry Steering Committee, p16 IHC Study Panel, Humans, Papillomavirus Infections, Cervical Intraepithelial Neoplasia, Immunohistochemistry, Adult, Middle Aged, Uterine Cervical Neoplasms, Female, Cyclin-Dependent Kinase Inhibitor p16, Biomarkers, Tumor, Pathology, Clinical Sciences

Abstract

Context.—Lower Anogenital Squamous Terminology (LAST) standardization recommended p16INK4a immunohistochemistry (p16 IHC) for biopsies diagnosed morphologically as cervical intraepithelial neoplasia (CIN) grade 2 (CIN2) to classify them as low-grade or high-grade squamous intraepithelial lesions (HSILs).Objective.—To describe the relationships of p16 IHC and other biomarkers associated with cervical cancer risk with biopsy diagnoses.Design.—A statewide, stratified sample of cervical biopsies diagnosed by community pathologists (CPs), including 1512 CIN2, underwent a consensus, expert pathologist panel (EP) review (without p16 IHC results), p16 IHC interpretation by a third pathology group, and human papillomavirus (HPV) genotyping, results of which were grouped hierarchically according to cancer risk. Antecedent cytologic interpretations were also available.Results.—Biopsies were more likely to test p16 IHC positive with increasing severity of CP diagnoses, overall (Ptrend ≤ .001) and within each HPV risk group (Ptrend ≤ .001 except for low-risk HPV [Ptrend < .010]). All abnormal grades of CP-diagnosed biopsies were more likely to test p16 IHC positive with a higher HPV risk group (Ptrend < .001), and testing p16 IHC positive was associated with higher HPV risk group than testing p16 IHC negative for each grade of CP-diagnosed biopsies (P < .001). p16 IHC-positive, CP-diagnosed CIN2 biopsies were less likely than CP-diagnosed CIN3 biopsies to test HPV16 positive, have an antecedent HSIL+ cytology, or to be diagnosed as CIN3+ by the EP (P < .001 for all). p16 IHC-positive, CP-diagnosed CIN1 biopsies had lower HPV risk groups than p16 IHC-negative, CP-diagnosed CIN2 biopsies (P < .001).Conclusions.—p16 IHC-positive, CP-diagnosed CIN2 appears to be lower cancer risk than CP-diagnosed CIN3. LAST classification of "HSIL" diagnosis, which includes p16 IHC-positive CIN2, should annotate the morphologic diagnosis (CIN2 or CIN3) to inform all management decisions, which is especially important for young (

Published

2020

15. Evaluation of TypeSeq, a Novel High-Throughput, Low-Cost, Next-Generation Sequencing-Based Assay for Detection of 51 Human Papillomavirus Genotypes

Author

Wagner, Sarah, Roberson, David, Boland, Joseph, Kreimer, Aimée R, Yeager, Meredith, Cullen, Michael, Mirabello, Lisa, Dunn, S Terence, Walker, Joan, Zuna, Rosemary, Porras, Carolina, Cortes, Bernal, Sampson, Joshua, Herrero, Rolando, Rodriguez, Ana Cecilia, Quint, Wim, Van Doorn, Leen-Jan, José, San, González, Paula, Jiménez, Silvia E, Rodríguez, Ana Cecilia, Hildesheim, Allan, Lowy, Douglas R, Schiffman, Mark, Schiller, John T, Sherman, Mark, Wacholder, Sholom, Pinto, Ligia A, Kemp, Troy J, Sidawy, Mary K, van Doorn, Leen-Jan, Struijk, Linda, Palefsky, Joel M, Darragh, Teresa M, Stoler, Mark H, and Wentzensen, Nicolas

Subjects

Reproductive Medicine, Biomedical and Clinical Sciences, Biological Sciences, Infectious Diseases, Prevention, Vaccine Related, Cervical Cancer, Biotechnology, Genetics, Cancer, HIV/AIDS, Sexually Transmitted Infections, Immunization, Adolescent, Adult, Aged, Aged, 80 and over, Costa Rica, Costs and Cost Analysis, Cross-Sectional Studies, Female, Genotype, Genotyping Techniques, High-Throughput Nucleotide Sequencing, Humans, Middle Aged, Papillomaviridae, Papillomavirus Infections, Papillomavirus Vaccines, Uterine Cervical Neoplasms, Young Adult, HPV, TypeSeq, vaccine efficacy, genotyping, screening, CVT Group, Medical and Health Sciences, Microbiology, Biological sciences, Biomedical and clinical sciences, Health sciences

Abstract

BackgroundHuman papillomaviruses (HPV) cause over 500 000 cervical cancers each year, most of which occur in low-resource settings. Human papillomavirus genotyping is important to study natural history and vaccine efficacy. We evaluated TypeSeq, a novel, next-generation, sequencing-based assay that detects 51 HPV genotypes, in 2 large international epidemiologic studies.MethodsTypeSeq was evaluated in 2804 cervical specimens from the Study to Understand Cervical Cancer Endpoints and Early Determinants (SUCCEED) and in 2357 specimens from the Costa Rica Vaccine Trial (CVT). Positive agreement and risks of precancer for individual genotypes were calculated for TypeSeq in comparison to Linear Array (SUCCEED). In CVT, positive agreement and vaccine efficacy were calculated for TypeSeq and SPF10-LiPA.ResultsWe observed high overall and positive agreement for most genotypes between TypeSeq and Linear Array in SUCCEED and SPF10-LiPA in CVT. There was no significant difference in risk of precancer between TypeSeq and Linear Array in SUCCEED or in estimates of vaccine efficacy between TypeSeq and SPF10-LiPA in CVT.ConclusionsThe agreement of TypeSeq with Linear Array and SPF10-LiPA, 2 well established standards for HPV genotyping, demonstrates its high accuracy. TypeSeq provides high-throughput, affordable HPV genotyping for world-wide studies of cervical precancer risk and of HPV vaccine efficacy.

Published

2019

16. Measurements of the separated longitudinal structure function FL from hydrogen and deuterium targets at low Q2

Author

Tvaskis, V, Tvaskis, A, Niculescu, I, Abbott, D, Adams, GS, Afanasev, A, Ahmidouch, A, Angelescu, T, Arrington, J, Asaturyan, R, Avery, S, Baker, OK, Benmouna, N, Berman, BL, Biselli, A, Blok, HP, Boeglin, WU, Bosted, PE, Brash, E, Breuer, H, Chang, G, Chant, N, Christy, ME, Connell, SH, Dalton, MM, Danagoulian, S, Day, D, Dodario, T, Dunne, JA, Dutta, D, El Khayari, N, Ent, R, Fenker, HC, Frolov, VV, Gaskell, D, Garrow, K, Gilman, R, Gueye, P, Hafidi, K, Hinton, W, Holt, RJ, Horn, T, Huber, GM, Jackson, H, Jiang, X, Jones, MK, Joo, K, Kelly, JJ, Keppel, CE, Kuhn, J, Kinney, E, Klein, A, Kubarovsky, V, Liang, Y, Lolos, G, Lung, A, Mack, D, Malace, S, Markowitz, P, Mbianda, G, McGrath, E, McKee, D, Meekins, DG, Mkrtchyan, H, Napolitano, J, Navasardyan, T, Niculescu, G, Nozar, M, Ostapenko, T, Papandreou, Z, Potterveld, D, Reimer, PE, Reinhold, J, Roche, J, Rock, SE, Schulte, E, Segbefia, E, Smith, C, Smith, GR, Stoler, P, Tadevosyan, V, Tang, L, Telfeyan, J, Todor, L, Ungaro, M, Uzzle, A, Vidakovic, S, Villano, A, Vulcan, WF, Warren, G, Wesselmann, F, Wojtsekhowski, B, Wood, SA, Yan, C, and Zihlmann, B

Abstract

Structure functions, as measured in lepton-nucleon scattering, have proven to be very useful in studying the partonic dynamics within the nucleon. However, it is experimentally difficult to separately determine the longitudinal and transverse structure functions, and consequently there are substantially less data available in particular for the longitudinal structure function. Here, we present separated structure functions for hydrogen and deuterium at low four-momentum transfer squared, Q2

Published

2018

17. Measurements of the separated longitudinal structure function FL from hydrogen and deuterium targets at low Q2

Author

Tvaskis, V, Tvaskis, A, Niculescu, I, Abbott, D, Adams, GS, Afanasev, A, Ahmidouch, A, Angelescu, T, Arrington, J, Asaturyan, R, Avery, S, Baker, OK, Benmouna, N, Berman, BL, Biselli, A, Blok, HP, Boeglin, WU, Bosted, PE, Brash, E, Breuer, H, Chang, G, Chant, N, Christy, ME, Connell, SH, Dalton, MM, Danagoulian, S, Day, D, Dodario, T, Dunne, JA, Dutta, D, Khayari, N El, Ent, R, Fenker, HC, Frolov, VV, Gaskell, D, Garrow, K, Gilman, R, Gueye, P, Hafidi, K, Hinton, W, Holt, RJ, Horn, T, Huber, GM, Jackson, H, Jiang, X, Jones, MK, Joo, K, Kelly, JJ, Keppel, CE, Kuhn, J, Kinney, E, Klein, A, Kubarovsky, V, Liang, Y, Lolos, G, Lung, A, Mack, D, Malace, S, Markowitz, P, Mbianda, G, McGrath, E, Mckee, D, Meekins, DG, Mkrtchyan, H, Napolitano, J, Navasardyan, T, Niculescu, G, Nozar, M, Ostapenko, T, Papandreou, Z, Potterveld, D, Reimer, PE, Reinhold, J, Roche, J, Rock, SE, Schulte, E, Segbefia, E, Smith, C, Smith, GR, Stoler, P, Tadevosyan, V, Tang, L, Telfeyan, J, Todor, L, Ungaro, M, Uzzle, A, Vidakovic, S, Villano, A, Vulcan, WF, Warren, G, Wesselmann, F, Wojtsekhowski, B, Wood, SA, Yan, C, and Zihlmann, B

Subjects

Nuclear and Plasma Physics, Particle and High Energy Physics, Synchrotrons and Accelerators, Physical Sciences, Nuclear and plasma physics

Abstract

Structure functions, as measured in lepton-nucleon scattering, have proven to be very useful in studying the partonic dynamics within the nucleon. However, it is experimentally difficult to separately determine the longitudinal and transverse structure functions, and consequently there are substantially less data available in particular for the longitudinal structure function. Here, we present separated structure functions for hydrogen and deuterium at low four-momentum transfer squared, Q2

Published

2018

18. Phylogenetic patterns of trait and trait plasticity evolution: Insights from amphibian embryos

Author

Relyea, Rick A, Stephens, Patrick R, Barrow, Lisa N, Blaustein, Andrew R, Bradley, Paul W, Buck, Julia C, Chang, Ann, Collins, James P, Crother, Brian, Earl, Julia, Gervasi, Stephanie S, Hoverman, Jason T, Hyman, Oliver, Lemmon, Emily Moriarty, Luhring, Thomas M, Michelson, Moses, Murray, Chris, Price, Steven, Semlitsch, Raymond D, Sih, Andrew, Stoler, Aaron B, VandenBroek, Nick, Warwick, Alexa, Wengert, Greta, and Hammond, John I

Subjects

Biological Sciences, Evolutionary Biology, Adaptation, Physiological, Animals, Anura, Astacoidea, Biological Evolution, Embryo, Nonmammalian, Food Chain, Life History Traits, Olfactory Perception, Phylogeny, United States, Anaxyrus, Hyla, Lithobates, Pseudacris, phylogenetic inertia, Rana, Ecology, Evolutionary biology

Abstract

Environmental variation favors the evolution of phenotypic plasticity. For many species, we understand the costs and benefits of different phenotypes, but we lack a broad understanding of how plastic traits evolve across large clades. Using identical experiments conducted across North America, we examined prey responses to predator cues. We quantified five life-history traits and the magnitude of their plasticity for 23 amphibian species/populations (spanning three families and five genera) when exposed to no cues, crushed-egg cues, and predatory crayfish cues. Embryonic responses varied considerably among species and phylogenetic signal was common among the traits, whereas phylogenetic signal was rare for trait plasticities. Among trait-evolution models, the Ornstein-Uhlenbeck (OU) model provided the best fit or was essentially tied with Brownian motion. Using the best fitting model, evolutionary rates for plasticities were higher than traits for three life-history traits and lower for two. These data suggest that the evolution of life-history traits in amphibian embryos is more constrained by a species' position in the phylogeny than is the evolution of life history plasticities. The fact that an OU model of trait evolution was often a good fit to patterns of trait variation may indicate adaptive optima for traits and their plasticities.

Published

2018

19. Durability of Protection Afforded by Fewer Doses of the HPV16/18 Vaccine: The CVT Trial

Author

Safaeian, Mahboobeh, Sampson, Joshua N, Pan, Yuanji, Porras, Carolina, Kemp, Troy J, Herrero, Rolando, Quint, Wim, van Doorn, Leen Jan, Schussler, John, Lowy, Douglas R, Schiller, John, Schiffman, Mark T, Rodriguez, Ana Cecilia, Gail, Mitchell H, Hildesheim, Allan, Gonzalez, Paula, Pinto, Ligia A, Kreimer, Aimée R, Paula, González, Jiménez, Silvia E, Rodríguez, Ana Cecilia, Schiffman, Mark, Schiller, John T, Sherman, Mark, Wacholder, Sholom, Sidawy, Mary K, van Doorn, Leen-Jan, Struijk, Linda, Palefsky, Joel M, Darragh, Teresa M, and Stoler, Mark H

Subjects

Immunization, Prevention, HPV and/or Cervical Cancer Vaccines, Biotechnology, Clinical Trials and Supportive Activities, Cervical Cancer, Clinical Research, Vaccine Related, Infectious Diseases, Sexually Transmitted Infections, Cancer, HIV/AIDS, Infection, Adolescent, Adult, Antibodies, Viral, Cervix Uteri, DNA, Viral, Female, Human papillomavirus 16, Human papillomavirus 18, Humans, Papillomavirus Infections, Papillomavirus Vaccines, Uterine Cervical Diseases, Young Adult, Costa Rica HPV Vaccine Trial (CVT) Group, Oncology and Carcinogenesis, Oncology & Carcinogenesis

Abstract

Previously, we demonstrated similar human papillomavirus (HPV)16/18 vaccine efficacy estimates and stable HPV16/18 antibody levels four years postvaccination in a nonrandomized analysis of women who received a varying number of doses of the bivalent HPV16/18 vaccine. Here we extend data to seven years following initial vaccination. We evaluated HPV16/18-vaccinated women who received one (n = 134), two (n 0/1 = 193, n 0/6 = 79), or three doses (n = 2043) to a median of 6.9 years postvaccination. Cervical HPV DNA was measured with the SPF10- DEIA-LiPA PCR system; HPV16/18-specific antibody levels were measured using enzyme-linked immunosorbent assays (n = 486). Infection and immunological measures were compared across vaccine dose groups. Prevalent HPV infection at year 7 was also compared with an unvaccinated control group (UCG). All statistical tests were two-sided. Among women in the three-dose, two-dose 0/6 , two-dose 0/1 , and one-dose groups, cumulative incident HPV16/18 infection rates (No. of events/No. of individuals) were 4.3% (88/2036, 95% confidence interval [CI] = 3.5% to 5.3%), 3.8% (3/78, 95% CI = 1.0% to 10.1%), 3.6% (7/192, 95% CI = 1.6% to 7.1%), and 1.5% (2/133, 95% CI = 0.3% to 4.9%; P = 1.00, .85, .17 comparing the two-dose 0/6 , two-dose 0/1 , and one-dose groups to the three-dose group, respectively). The prevalence of other carcinogenic and noncarcinogenic HPV types, excluding HPV16/18/31/33/45, were high and not statistically different among all dose groups, indicating that the low incidence of HPV16/18 in the one- and two-dose groups was not due to lack of exposure. At seven years, 100% of participants in all dose groups remained HPV16 and HPV18 seropositive. A non-statistically significant decrease in the geometric mean of the HPV16 antibody levels between years 4 and 7 was observed among women in the three-dose group: -10.8% (95% CI = -25.3% to 6.6%); two-dose (0/6 months) group: -17.3% (95% CI = -39.3% to 12.8%), two-dose (0/1 month) group: -6.9% (95% CI = -22.1% to 11.2%), and one-dose group: -5.5% (95% CI = -29.7% to 27.0%); results were similar for HPV18. At an average of seven years of follow-up, we observed similar low rates of HPV16/18 infections and slight, if any, decreases in HPV16/18 antibody levels by dose group.

Published

2018

20. An integrated clinical program and crowdsourcing strategy for genomic sequencing and Mendelian disease gene discovery

Author

Haghighi, Alireza, Krier, Joel B, Toth-Petroczy, Agnes, Cassa, Christopher A, Frank, Natasha Y, Carmichael, Nikkola, Fieg, Elizabeth, Bjonnes, Andrew, Mohanty, Anwoy, Briere, Lauren C, Lincoln, Sharyn, Lucia, Stephanie, Gupta, Vandana A, Söylemez, Onuralp, Sutti, Sheila, Kooshesh, Kameron, Qiu, Haiyan, Fay, Christopher J, Perroni, Victoria, Valerius, Jamie, Hanna, Meredith, Frank, Alexander, Ouahed, Jodie, Snapper, Scott B, Pantazi, Angeliki, Chopra, Sameer S, Leshchiner, Ignaty, Stitziel, Nathan O, Feldweg, Anna, Mannstadt, Michael, Loscalzo, Joseph, Sweetser, David A, Liao, Eric, Stoler, Joan M, Nowak, Catherine B, Sanchez-Lara, Pedro A, Klein, Ophir D, Perry, Hazel, Patsopoulos, Nikolaos A, Raychaudhuri, Soumya, Goessling, Wolfram, Green, Robert C, Seidman, Christine E, MacRae, Calum A, Sunyaev, Shamil R, Maas, Richard L, Vuzman, Dana, and Undiagnosed Diseases Network, Brigham and Women’s Hospital FaceBase Project, Brigham Genomic Medicine (BGM)

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Genetics, Human Genome, Biotechnology, Clinical Research, 2.1 Biological and endogenous factors, Aetiology, Good Health and Well Being, Undiagnosed Diseases Network, Brigham and Women’s Hospital FaceBase Project, Brigham Genomic Medicine, Medical biotechnology

Abstract

Despite major progress in defining the genetic basis of Mendelian disorders, the molecular etiology of many cases remains unknown. Patients with these undiagnosed disorders often have complex presentations and require treatment by multiple health care specialists. Here, we describe an integrated clinical diagnostic and research program using whole-exome and whole-genome sequencing (WES/WGS) for Mendelian disease gene discovery. This program employs specific case ascertainment parameters, a WES/WGS computational analysis pipeline that is optimized for Mendelian disease gene discovery with variant callers tuned to specific inheritance modes, an interdisciplinary crowdsourcing strategy for genomic sequence analysis, matchmaking for additional cases, and integration of the findings regarding gene causality with the clinical management plan. The interdisciplinary gene discovery team includes clinical, computational, and experimental biomedical specialists who interact to identify the genetic etiology of the disease, and when so warranted, to devise improved or novel treatments for affected patients. This program effectively integrates the clinical and research missions of an academic medical center and affords both diagnostic and therapeutic options for patients suffering from genetic disease. It may therefore be germane to other academic medical institutions engaged in implementing genomic medicine programs.

Published

2018

21. An integrated clinical program and crowdsourcing strategy for genomic sequencing and Mendelian disease gene discovery.

Author

Haghighi, Alireza, Krier, Joel B, Toth-Petroczy, Agnes, Cassa, Christopher A, Frank, Natasha Y, Carmichael, Nikkola, Fieg, Elizabeth, Bjonnes, Andrew, Mohanty, Anwoy, Briere, Lauren C, Lincoln, Sharyn, Lucia, Stephanie, Gupta, Vandana A, Söylemez, Onuralp, Sutti, Sheila, Kooshesh, Kameron, Qiu, Haiyan, Fay, Christopher J, Perroni, Victoria, Valerius, Jamie, Hanna, Meredith, Frank, Alexander, Ouahed, Jodie, Snapper, Scott B, Pantazi, Angeliki, Chopra, Sameer S, Leshchiner, Ignaty, Stitziel, Nathan O, Feldweg, Anna, Mannstadt, Michael, Loscalzo, Joseph, Sweetser, David A, Liao, Eric, Stoler, Joan M, Nowak, Catherine B, Sanchez-Lara, Pedro A, Klein, Ophir D, Perry, Hazel, Patsopoulos, Nikolaos A, Raychaudhuri, Soumya, Goessling, Wolfram, Green, Robert C, Seidman, Christine E, MacRae, Calum A, Sunyaev, Shamil R, Maas, Richard L, Vuzman, Dana, and Undiagnosed Diseases Network, Brigham and Women’s Hospital FaceBase Project, Brigham Genomic Medicine (BGM)

Subjects

Undiagnosed Diseases Network, Brigham and Women’s Hospital FaceBase Project, Brigham Genomic Medicine, Undiagnosed Diseases Network, Brigham and Women’s Hospital FaceBase Project, Brigham Genomic Medicine

Abstract

Despite major progress in defining the genetic basis of Mendelian disorders, the molecular etiology of many cases remains unknown. Patients with these undiagnosed disorders often have complex presentations and require treatment by multiple health care specialists. Here, we describe an integrated clinical diagnostic and research program using whole-exome and whole-genome sequencing (WES/WGS) for Mendelian disease gene discovery. This program employs specific case ascertainment parameters, a WES/WGS computational analysis pipeline that is optimized for Mendelian disease gene discovery with variant callers tuned to specific inheritance modes, an interdisciplinary crowdsourcing strategy for genomic sequence analysis, matchmaking for additional cases, and integration of the findings regarding gene causality with the clinical management plan. The interdisciplinary gene discovery team includes clinical, computational, and experimental biomedical specialists who interact to identify the genetic etiology of the disease, and when so warranted, to devise improved or novel treatments for affected patients. This program effectively integrates the clinical and research missions of an academic medical center and affords both diagnostic and therapeutic options for patients suffering from genetic disease. It may therefore be germane to other academic medical institutions engaged in implementing genomic medicine programs.

Published

2018

22. Impact of human papillomavirus (HPV) 16 and 18 vaccination on prevalent infections and rates of cervical lesions after excisional treatment

Author

Hildesheim, Allan, Gonzalez, Paula, Kreimer, Aimee R, Wacholder, Sholom, Schussler, John, Rodriguez, Ana C, Porras, Carolina, Schiffman, Mark, Sidawy, Mary, Schiller, John T, Lowy, Douglas R, Herrero, Rolando, Group, Costa Rica HPV Vaccine Trial, Cortés, Bernal, González, Paula, Herrero, Roland, Jiménez, Silvia E, Rodríguez, Ana Cecilia, Kreimer, Aimée R, Sherman, Mark, Pinto, Ligia, Kemp, Troy, Quint, Wim, van Doorn, Leen-Jan, Palefsky, Joel M, Darragh, Teresa M, and Stoler, Mark H

Subjects

Reproductive Medicine, Biomedical and Clinical Sciences, Infectious Diseases, Cervical Cancer, HPV and/or Cervical Cancer Vaccines, Cancer, HIV/AIDS, Clinical Trials and Supportive Activities, Vaccine Related, Sexually Transmitted Infections, Prevention, Immunization, Clinical Research, 3.4 Vaccines, Prevention of disease and conditions, and promotion of well-being, Infection, Good Health and Well Being, Adolescent, Adult, Cervix Uteri, Female, Human papillomavirus 16, Human papillomavirus 18, Humans, Incidence, Papillomavirus Infections, Papillomavirus Vaccines, Prevalence, Treatment Outcome, Uterine Cervical Neoplasms, Vaccination, Young Adult, Uterine Cervical Dysplasia, Costa Rica HPV Vaccine Trial (CVT) Group, cervical cancer, clinical trial, human papillomaviruses, prevention, vaccines, Paediatrics and Reproductive Medicine, Obstetrics & Reproductive Medicine, Reproductive medicine

Abstract

BackgroundHuman papillomavirus vaccines prevent human papillomavirus infection and cervical precancers. The impact of vaccinating women with a current infection or after treatment for an human papillomavirus-associated lesion is not fully understood.ObjectivesTo determine whether human papillomavirus-16/18 vaccination influences the outcome of infections present at vaccination and the rate of infection and disease after treatment of lesions.Study designWe included 1711 women (18-25 years) with carcinogenic human papillomavirus infection and 311 women of similar age who underwent treatment for cervical precancer and who participated in a community-based trial of the AS04-adjuvanted human papillomavirus-16/18 virus-like particle vaccine. Participants were randomized (human papillomavirus or hepatitis A vaccine) and offered 3 vaccinations over 6 months. Follow-up included annual visits (more frequently if clinically indicated), referral to colposcopy of high-grade and persistent low-grade lesions, treatment by loop electrosurgical excisional procedure when clinically indicated, and cytologic and virologic follow-up after treatment. Among women with human papillomavirus infection at the time of vaccination, we considered type-specific viral clearance, and development of cytologic (squamous intraepithelial lesions) and histologic (cervical intraepithelial neoplasia) lesions. Among treated women, we considered single-time and persistent human papillomavirus infection, squamous intraepithelial lesions, and cervical intraepithelial neoplasia 2 or greater. Outcomes associated with infections absent before treatment also were evaluated. Infection-level analyses were performed and vaccine efficacy estimated.ResultsMedian follow-up was 56.7 months (women with human papillomavirus infection) and 27.3 months (treated women). There was no evidence of vaccine efficacy to increase clearance of human papillomavirus infections or decrease incidence of cytologic/histologic abnormalities associated with human papillomavirus types present at enrollment. Vaccine efficacy for human papillomavirus 16/18 clearance and against human papillomavirus 16/18 progression from infection to cervical intraepithelial neoplasia 2 or greater were -5.4% (95% confidence interval -19,10) and 0.3% (95% confidence interval -69,41), respectively. Among treated women, 34.1% had oncogenic infection and 1.6% had cervical intraepithelial neoplasia 2 or greater detected after treatment, respectively, and of these 69.8% and 20.0% were the result of new infections. We observed no significant effect of vaccination on rates of infection/lesions after treatment. Vaccine efficacy estimates for human papillomavirus 16/18 associated persistent infection and cervical intraepithelial neoplasia 2 or greater after treatment were 34.7% (95% confidence interval -131, 82) and -211% (95% confidence interval -2901, 68), respectively. We observed evidence for a partial and nonsignificant protective effect of vaccination against new infections absent before treatment. For incident human papillomavirus 16/18, human papillomavirus 31/33/45, and oncogenic human papillomavirus infections post-treatment, vaccine efficacy estimates were 57.9% (95% confidence interval -43, 88), 72.9% (95% confidence interval 29, 90), and 36.7% (95% confidence interval 1.5, 59), respectively.ConclusionWe find no evidence for a vaccine effect on the fate of detectable human papillomavirus infections. We show that vaccination does not protect against infections/lesions after treatment. Evaluation of vaccine protection against new infections after treatment and resultant lesions warrants further consideration in future studies.

Published

2016

23. Cross-protection of the Bivalent Human Papillomavirus (HPV) Vaccine Against Variants of Genetically Related High-Risk HPV Infections

Author

Harari, Ariana, Chen, Zigui, Rodríguez, Ana Cecilia, Hildesheim, Allan, Porras, Carolina, Herrero, Rolando, Wacholder, Sholom, Panagiotou, Orestis A, Befano, Brian, Burk, Robert D, Schiffman, Mark, González, Paula, Herrero, Roland, Jiménez, Silvia E, Kreimer, Aimée R, Lowy, Douglas R, Schiller, John T, Sherman, Mark, Pinto, Ligia A, Kemp, Troy J, Sidawy, Mary, Quint, Wim, van Doorn, Leen-Jan, Struijk, Linda, Palefsky, Joel M, Darragh, Teresa M, and Stoler, Mark H

Subjects

HIV/AIDS, Immunization, HPV and/or Cervical Cancer Vaccines, Cervical Cancer, Vaccine Related, Cancer, Infectious Diseases, Prevention, Genetics, Sexually Transmitted Infections, Aetiology, 2.1 Biological and endogenous factors, Infection, Adolescent, Adult, Double-Blind Method, Female, Genetic Variation, Humans, Papillomaviridae, Papillomavirus Infections, Papillomavirus Vaccines, Young Adult, Costa Rica HPV Vaccine Trial Group, HPV vaccine, HPV variants, cross-protection, Biological Sciences, Medical and Health Sciences, Microbiology

Abstract

BackgroundResults from the Costa Rica Vaccine Trial (CVT) demonstrated partial cross-protection by the bivalent human papillomavirus (HPV) vaccine, which targets HPV-16 and HPV-18, against HPV-31, -33, and -45 infection and an increased incidence of HPV-51 infection.MethodsA study nested within the CVT intention-to-treat cohort was designed to assess high-risk HPV variant lineage-specific vaccine efficacy (VE). The 2 main end points were (1) long-term incident infections persisting for ≥2 years and/or progression to high-grade squamous intraepithelial lesions (ie, cervical intraepithelial neoplasia grade 2/3 [CIN 2/3]) and (2) incident transient infections lasting for

Published

2016

24. Waterproofed photomultiplier tube assemblies for the Daya Bay reactor neutrino experiment

Author

Chow, Ken, Cummings, John, Edwards, Emily, Edwards, William, Ely, Ry, Hoff, Matthew, Lebanowski, Logan, Li, Bo, Li, Piyi, Lin, Shih-Kai, Liu, Dawei, Liu, Jinchang, Luk, Kam-Biu, Miao, Jiayuan, Napolitano, Jim, Ochoa-Ricoux, Juan Pedro, Peng, Jen-Chieh, Qi, Ming, Steiner, Herbert, Stoler, Paul, Stuart, Mary, Wang, Lingyu, Yang, Changgen, and Zhong, Weili

Subjects

Daya Bay, Reactor, Anti-neutrino, Waterproof, Photomultiplier tube, MACRO, physics.ins-det, hep-ex, Astronomical and Space Sciences, Atomic, Molecular, Nuclear, Particle and Plasma Physics, Other Physical Sciences, Nuclear & Particles Physics

Abstract

Abstract In the Daya Bay Reactor Neutrino Experiment 960 20-cm-diameter waterproof photomultiplier tubes are used to instrument three water pools as Cherenkov detectors for detecting cosmic-ray muons. Of these 960 photomultiplier tubes, 341 are recycled from the MACRO experiment. A systematic program was undertaken to refurbish them as waterproof assemblies. In the context of passing the water leakage check, a success rate better than 97% was achieved. Details of the design, fabrication, testing, operation, and performance of these waterproofed photomultiplier-tube assemblies are presented.

Published

2015

25. Waterproofed photomultiplier tube assemblies for the Daya Bay reactor neutrino experiment

Author

Chow, K, Cummings, J, Edwards, E, Edwards, W, Ely, R, Hoff, M, Lebanowski, L, Li, B, Li, P, Lin, SK, Liu, D, Liu, J, Luk, KB, Miao, J, Napolitano, J, Ochoa-Ricoux, JP, Peng, JC, Qi, M, Steiner, H, Stoler, P, Stuart, M, Wang, L, Yang, C, and Zhong, W

Subjects

Daya Bay, Reactor, Anti-neutrino, Waterproof, Photomultiplier tube, MACRO, physics.ins-det, hep-ex, Nuclear & Particles Physics, Astronomical and Space Sciences, Atomic, Molecular, Nuclear, Particle and Plasma Physics, Other Physical Sciences

Abstract

Abstract In the Daya Bay Reactor Neutrino Experiment 960 20-cm-diameter waterproof photomultiplier tubes are used to instrument three water pools as Cherenkov detectors for detecting cosmic-ray muons. Of these 960 photomultiplier tubes, 341 are recycled from the MACRO experiment. A systematic program was undertaken to refurbish them as waterproof assemblies. In the context of passing the water leakage check, a success rate better than 97% was achieved. Details of the design, fabrication, testing, operation, and performance of these waterproofed photomultiplier-tube assemblies are presented.

Published

2015

26. Mutations in PYCR2, Encoding Pyrroline-5-Carboxylate Reductase 2, Cause Microcephaly and Hypomyelination

Author

Nakayama, Tojo, Al-Maawali, Almundher, El-Quessny, Malak, Rajab, Anna, Khalil, Samir, Stoler, Joan M, Tan, Wen-Hann, Nasir, Ramzi, Schmitz-Abe, Klaus, Hill, R Sean, Partlow, Jennifer N, Al-Saffar, Muna, Servattalab, Sarah, LaCoursiere, Christopher M, Tambunan, Dimira E, Coulter, Michael E, Elhosary, Princess C, Gorski, Grzegorz, Barkovich, A James, Markianos, Kyriacos, Poduri, Annapurna, and Mochida, Ganeshwaran H

Subjects

Biochemistry and Cell Biology, Bioinformatics and Computational Biology, Genetics, Biological Sciences, Neurosciences, Human Genome, Brain Disorders, Intellectual and Developmental Disabilities (IDD), Clinical Research, Congenital Structural Anomalies, Rare Diseases, Pediatric, Aetiology, 2.1 Biological and endogenous factors, Generic health relevance, Amino Acid Transport Systems, Acidic, Antiporters, Female, Genotype, Hereditary Central Nervous System Demyelinating Diseases, Homozygote, Humans, Male, Microcephaly, Mitochondrial Diseases, Mutation, Phenotype, Psychomotor Disorders, Pyrroline Carboxylate Reductases, Medical and Health Sciences, Genetics & Heredity, Biological sciences, Biomedical and clinical sciences, Health sciences

Abstract

Despite recent advances in understanding the genetic bases of microcephaly, a large number of cases of microcephaly remain unexplained, suggesting that many microcephaly syndromes and associated genes have yet to be identified. Here, we report mutations in PYCR2, which encodes an enzyme in the proline biosynthesis pathway, as the cause of a unique syndrome characterized by postnatal microcephaly, hypomyelination, and reduced cerebral white-matter volume. Linkage mapping and whole-exome sequencing identified homozygous mutations (c.355C>T [p.Arg119Cys] and c.751C>T [p.Arg251Cys]) in PYCR2 in the affected individuals of two consanguineous families. A lymphoblastoid cell line from one affected individual showed a strong reduction in the amount of PYCR2. When mutant cDNAs were transfected into HEK293FT cells, both variant proteins retained normal mitochondrial localization but had lower amounts than the wild-type protein, suggesting that the variant proteins were less stable. A PYCR2-deficient HEK293FT cell line generated by genome editing with the clustered regularly interspaced short palindromic repeat (CRISPR)-Cas9 system showed that PYCR2 loss of function led to decreased mitochondrial membrane potential and increased susceptibility to apoptosis under oxidative stress. Morpholino-based knockdown of a zebrafish PYCR2 ortholog, pycr1b, recapitulated the human microcephaly phenotype, which was rescued by wild-type human PYCR2 mRNA, but not by mutant mRNAs, further supporting the pathogenicity of the identified variants. Hypomyelination and the absence of lax, wrinkly skin distinguishes this condition from that caused by previously reported mutations in the gene encoding PYCR2's isozyme, PYCR1, suggesting a unique and indispensable role for PYCR2 in the human CNS during development.

Published

2015

27. Rationale and design of a long term follow-up study of women who did and did not receive HPV 16/18 vaccination in Guanacaste, Costa Rica.

Author

Gonzalez, Paula, Hildesheim, Allan, Herrero, Rolando, Katki, Hormuzd, Wacholder, Sholom, Porras, Carolina, Safaeian, Mahboobeh, Jimenez, Silvia, Schiller, John, Ocampo, Rebeca, Schussler, John, Lowy, Douglas, Guillen, Diego, Stoler, Mark, Quint, Wim, Morales, Jorge, Avila, Carlos, Rodriguez, Ana, Kreimer, Aimée, Cortes, Bernal, Befano, Brian, Schiffman, Mark, Carvajal, Loreto, Palefsky, Joel, and Darragh, Teresa

Subjects

Human papillomavirus, Long term follow-up, Methods, Vaccines, Adult, Costa Rica, Cross-Over Studies, Early Detection of Cancer, Female, Follow-Up Studies, Hepatitis A Vaccines, Human papillomavirus 16, Human papillomavirus 18, Humans, Papillomavirus Infections, Papillomavirus Vaccines, Research Design, Time Factors, Uterine Cervical Diseases, Uterine Cervical Neoplasms, Vaccination, Young Adult, Uterine Cervical Dysplasia

Abstract

The Costa Rica Vaccine Trial (CVT) was a randomized clinical trial conducted between 2004 and 2010, which randomized 7466 women aged 18 to 25 to receive the bivalent HPV-16/18 vaccine or control Hepatitis-A vaccine. Participants were followed for 4 years with cross-over vaccination at the study end. In 2010 the long term follow-up (LTFU) study was initiated to evaluate the 10-year impact of HPV-16/18 vaccination, determinants of the immune response, and HPV natural history in a vaccinated population. Herein, the rationale, design and methods of the LTFU study are described, which actively follows CVT participants in the HPV-arm 6 additional years at biennial intervals (3 additional study visits for 10 years of total follow-up), or more often if clinically indicated. According to the initial commitment, women in the Hepatitis-A arm were offered HPV vaccination at cross-over; they were followed 2 additional years and exited from the study. 92% of eligible CVT women accepted participation in LTFU. To provide underlying rates of HPV acquisition and cervical disease among unvaccinated women to compare with the HPV-arm during LTFU, a new unvaccinated control group (UCG) of women who are beyond the age generally recommended for routine vaccination was enrolled, and will be followed by cervical cancer screening over 6 years. To form the UCG, 5000 women were selected from a local census, of whom 2836 women (61% of eligible women) agreed to participate. Over 90% of participants complied with an interview, blood and cervical specimen collection. Evaluation of comparability between the original (Hepatitis-A arm of CVT) and new (UCG) control groups showed that womens characteristics, as well as their predicted future risk for cervical HPV acquisition, were similar, thus validating use of the UCG. LTFU is poised to comprehensively address many important questions related to long-term effects of prophylactic HPV vaccines.

Published

2015

28. Rationale and design of a long term follow-up study of women who did and did not receive HPV 16/18 vaccination in Guanacaste, Costa Rica.

Author

Gonzalez, Paula, Hildesheim, Allan, Herrero, Rolando, Katki, Hormuzd, Wacholder, Sholom, Porras, Carolina, Safaeian, Mahboobeh, Jimenez, Silvia, Darragh, Teresa M, Cortes, Bernal, Befano, Brian, Schiffman, Mark, Carvajal, Loreto, Palefsky, Joel, Schiller, John, Ocampo, Rebeca, Schussler, John, Lowy, Douglas, Guillen, Diego, Stoler, Mark H, Quint, Wim, Morales, Jorge, Avila, Carlos, Rodriguez, Ana Cecilia, Kreimer, Aimée R, and Costa Rica HPV Vaccine Trial (CVT) Group

Subjects

Costa Rica HPV Vaccine Trial (CVT) Group, Humans, Papillomavirus Infections, Hepatitis A Vaccines, Vaccination, Follow-Up Studies, Cross-Over Studies, Research Design, Time Factors, Adult, Costa Rica, Uterine Cervical Diseases, Uterine Cervical Dysplasia, Uterine Cervical Neoplasms, Female, Human papillomavirus 18, Human papillomavirus 16, Papillomavirus Vaccines, Early Detection of Cancer, Young Adult, Human papillomavirus, Long term follow-up, Methods, Vaccines, Digestive Diseases, Cervical Cancer, Cancer, Clinical Research, Biotechnology, HIV/AIDS, Immunization, HPV and/or Cervical Cancer Vaccines, Prevention, Vaccine Related, Clinical Trials and Supportive Activities, Infectious Diseases, Sexually Transmitted Infections, Evaluation of treatments and therapeutic interventions, 3.4 Vaccines, Prevention of disease and conditions, and promotion of well-being, 6.1 Pharmaceuticals, Infection, Good Health and Well Being, Cervical Intraepithelial Neoplasia, Biological Sciences, Agricultural and Veterinary Sciences, Medical and Health Sciences, Virology

Abstract

The Costa Rica Vaccine Trial (CVT) was a randomized clinical trial conducted between 2004 and 2010, which randomized 7466 women aged 18 to 25 to receive the bivalent HPV-16/18 vaccine or control Hepatitis-A vaccine. Participants were followed for 4 years with cross-over vaccination at the study end. In 2010 the long term follow-up (LTFU) study was initiated to evaluate the 10-year impact of HPV-16/18 vaccination, determinants of the immune response, and HPV natural history in a vaccinated population. Herein, the rationale, design and methods of the LTFU study are described, which actively follows CVT participants in the HPV-arm 6 additional years at biennial intervals (3 additional study visits for 10 years of total follow-up), or more often if clinically indicated. According to the initial commitment, women in the Hepatitis-A arm were offered HPV vaccination at cross-over; they were followed 2 additional years and exited from the study. 92% of eligible CVT women accepted participation in LTFU. To provide underlying rates of HPV acquisition and cervical disease among unvaccinated women to compare with the HPV-arm during LTFU, a new unvaccinated control group (UCG) of women who are beyond the age generally recommended for routine vaccination was enrolled, and will be followed by cervical cancer screening over 6 years. To form the UCG, 5000 women were selected from a local census, of whom 2836 women (61% of eligible women) agreed to participate. Over 90% of participants complied with an interview, blood and cervical specimen collection. Evaluation of comparability between the original (Hepatitis-A arm of CVT) and new (UCG) control groups showed that women's characteristics, as well as their predicted future risk for cervical HPV acquisition, were similar, thus validating use of the UCG. LTFU is poised to comprehensively address many important questions related to long-term effects of prophylactic HPV vaccines.

Published

2015

29. Rationale and design of a long term follow-up study of women who did and did not receive HPV 16/18 vaccination in Guanacaste, Costa Rica.

Author

Gonzalez, Paula, Hildesheim, Allan, Herrero, Rolando, Katki, Hormuzd, Wacholder, Sholom, Porras, Carolina, Safaeian, Mahboobeh, Jimenez, Silvia, Darragh, Teresa M, Cortes, Bernal, Befano, Brian, Schiffman, Mark, Carvajal, Loreto, Palefsky, Joel, Schiller, John, Ocampo, Rebeca, Schussler, John, Lowy, Douglas, Guillen, Diego, Stoler, Mark H, Quint, Wim, Morales, Jorge, Avila, Carlos, Rodriguez, Ana Cecilia, Kreimer, Aimée R, and Costa Rica HPV Vaccine Trial (CVT) Group

Subjects

Costa Rica HPV Vaccine Trial (CVT) Group, Humans, Papillomavirus Infections, Cervical Intraepithelial Neoplasia, Hepatitis A Vaccines, Vaccination, Follow-Up Studies, Cross-Over Studies, Research Design, Time Factors, Adult, Costa Rica, Uterine Cervical Diseases, Uterine Cervical Neoplasms, Female, Human papillomavirus 18, Human papillomavirus 16, Papillomavirus Vaccines, Early Detection of Cancer, Young Adult, Human papillomavirus, Long term follow-up, Methods, Vaccines, Cervical Cancer, Prevention, Cancer, HPV and/or Cervical Cancer Vaccines, Clinical Research, Vaccine Related, Digestive Diseases, Infectious Diseases, Clinical Trials and Supportive Activities, Biotechnology, Immunization, Sexually Transmitted Infections, HIV/AIDS, 3.4 Vaccines, 6.1 Pharmaceuticals, Infection, Virology, Biological Sciences, Agricultural and Veterinary Sciences, Medical and Health Sciences

Abstract

The Costa Rica Vaccine Trial (CVT) was a randomized clinical trial conducted between 2004 and 2010, which randomized 7466 women aged 18 to 25 to receive the bivalent HPV-16/18 vaccine or control Hepatitis-A vaccine. Participants were followed for 4 years with cross-over vaccination at the study end. In 2010 the long term follow-up (LTFU) study was initiated to evaluate the 10-year impact of HPV-16/18 vaccination, determinants of the immune response, and HPV natural history in a vaccinated population. Herein, the rationale, design and methods of the LTFU study are described, which actively follows CVT participants in the HPV-arm 6 additional years at biennial intervals (3 additional study visits for 10 years of total follow-up), or more often if clinically indicated. According to the initial commitment, women in the Hepatitis-A arm were offered HPV vaccination at cross-over; they were followed 2 additional years and exited from the study. 92% of eligible CVT women accepted participation in LTFU. To provide underlying rates of HPV acquisition and cervical disease among unvaccinated women to compare with the HPV-arm during LTFU, a new unvaccinated control group (UCG) of women who are beyond the age generally recommended for routine vaccination was enrolled, and will be followed by cervical cancer screening over 6 years. To form the UCG, 5000 women were selected from a local census, of whom 2836 women (61% of eligible women) agreed to participate. Over 90% of participants complied with an interview, blood and cervical specimen collection. Evaluation of comparability between the original (Hepatitis-A arm of CVT) and new (UCG) control groups showed that women's characteristics, as well as their predicted future risk for cervical HPV acquisition, were similar, thus validating use of the UCG. LTFU is poised to comprehensively address many important questions related to long-term effects of prophylactic HPV vaccines.

Published

2015

30. Maternal age effect and severe germ-line bottleneck in the inheritance of human mitochondrial DNA

Author

Rebolledo-Jaramillo, Boris, Su, Marcia Shu-Wei, Stoler, Nicholas, McElhoe, Jennifer A, Dickins, Benjamin, Blankenberg, Daniel, Korneliussen, Thorfinn S, Chiaromonte, Francesca, Nielsen, Rasmus, Holland, Mitchell M, Paul, Ian M, Nekrutenko, Anton, and Makova, Kateryna D

Subjects

Biological Sciences, Genetics, Prevention, Age Factors, Child, DNA, Mitochondrial, Disease, Female, Gene Frequency, Germ Cells, Humans, INDEL Mutation, Inheritance Patterns, Maternal Age, Reproducibility of Results, Sequence Analysis, DNA, mitochondria, heteroplasmy

Abstract

The manifestation of mitochondrial DNA (mtDNA) diseases depends on the frequency of heteroplasmy (the presence of several alleles in an individual), yet its transmission across generations cannot be readily predicted owing to a lack of data on the size of the mtDNA bottleneck during oogenesis. For deleterious heteroplasmies, a severe bottleneck may abruptly transform a benign (low) frequency in a mother into a disease-causing (high) frequency in her child. Here we present a high-resolution study of heteroplasmy transmission conducted on blood and buccal mtDNA of 39 healthy mother-child pairs of European ancestry (a total of 156 samples, each sequenced at ∼20,000× per site). On average, each individual carried one heteroplasmy, and one in eight individuals carried a disease-associated heteroplasmy, with minor allele frequency ≥1%. We observed frequent drastic heteroplasmy frequency shifts between generations and estimated the effective size of the germ-line mtDNA bottleneck at only ∼30-35 (interquartile range from 9 to 141). Accounting for heteroplasmies, we estimated the mtDNA germ-line mutation rate at 1.3 × 10(-8) (interquartile range from 4.2 × 10(-9) to 4.1 × 10(-8)) mutations per site per year, an order of magnitude higher than for nuclear DNA. Notably, we found a positive association between the number of heteroplasmies in a child and maternal age at fertilization, likely attributable to oocyte aging. This study also took advantage of droplet digital PCR (ddPCR) to validate heteroplasmies and confirm a de novo mutation. Our results can be used to predict the transmission of disease-causing mtDNA variants and illuminate evolutionary dynamics of the mitochondrial genome.

Published

2014

31. Maternal age effect and severe germ-line bottleneck in the inheritance of human mitochondrial DNA.

Author

Rebolledo-Jaramillo, Boris, Su, Marcia Shu-Wei, Stoler, Nicholas, McElhoe, Jennifer A, Dickins, Benjamin, Blankenberg, Daniel, Korneliussen, Thorfinn S, Chiaromonte, Francesca, Nielsen, Rasmus, Holland, Mitchell M, Paul, Ian M, Nekrutenko, Anton, and Makova, Kateryna D

Subjects

Germ Cells, Humans, Disease, DNA, Mitochondrial, Reproducibility of Results, Sequence Analysis, DNA, Age Factors, Maternal Age, Gene Frequency, Inheritance Patterns, Child, Female, INDEL Mutation, heteroplasmy, mitochondria, Prevention, Genetics

Abstract

The manifestation of mitochondrial DNA (mtDNA) diseases depends on the frequency of heteroplasmy (the presence of several alleles in an individual), yet its transmission across generations cannot be readily predicted owing to a lack of data on the size of the mtDNA bottleneck during oogenesis. For deleterious heteroplasmies, a severe bottleneck may abruptly transform a benign (low) frequency in a mother into a disease-causing (high) frequency in her child. Here we present a high-resolution study of heteroplasmy transmission conducted on blood and buccal mtDNA of 39 healthy mother-child pairs of European ancestry (a total of 156 samples, each sequenced at ∼20,000× per site). On average, each individual carried one heteroplasmy, and one in eight individuals carried a disease-associated heteroplasmy, with minor allele frequency ≥1%. We observed frequent drastic heteroplasmy frequency shifts between generations and estimated the effective size of the germ-line mtDNA bottleneck at only ∼30-35 (interquartile range from 9 to 141). Accounting for heteroplasmies, we estimated the mtDNA germ-line mutation rate at 1.3 × 10(-8) (interquartile range from 4.2 × 10(-9) to 4.1 × 10(-8)) mutations per site per year, an order of magnitude higher than for nuclear DNA. Notably, we found a positive association between the number of heteroplasmies in a child and maternal age at fertilization, likely attributable to oocyte aging. This study also took advantage of droplet digital PCR (ddPCR) to validate heteroplasmies and confirm a de novo mutation. Our results can be used to predict the transmission of disease-causing mtDNA variants and illuminate evolutionary dynamics of the mitochondrial genome.

Published

2014

32. Deletions in GRID2 lead to a recessive syndrome of cerebellar ataxia and tonic upgaze in humans

Author

Hills, L Benjamin, Masri, Amira, Konno, Kotaro, Kakegawa, Wataru, Lam, Anh-Thu N, Lim-Melia, Elizabeth, Chandy, Nandini, Hill, R Sean, Partlow, Jennifer N, Al-Saffar, Muna, Nasir, Ramzi, Stoler, Joan M, Barkovich, A James, Watanabe, Masahiko, Yuzaki, Michisuke, and Mochida, Ganeshwaran H

Subjects

Rare Diseases, Neurosciences, Clinical Research, Pediatric, Brain Disorders, Genetics, 2.1 Biological and endogenous factors, Aetiology, Neurological, Adolescent, Animals, Cerebellar Ataxia, Child, Child, Preschool, Exons, Female, Genes, Recessive, Humans, Male, Mice, Ocular Motility Disorders, Receptors, Glutamate, Sequence Deletion, Syndrome, Clinical Sciences, Cognitive Sciences, Neurology & Neurosurgery

Abstract

ObjectiveTo identify the genetic cause of a syndrome causing cerebellar ataxia and eye movement abnormalities.MethodsWe identified 2 families with cerebellar ataxia, eye movement abnormalities, and global developmental delay. We performed genetic analyses including single nucleotide polymorphism genotyping, linkage analysis, array comparative genomic hybridization, quantitative PCR, and Sanger sequencing. We obtained eye movement recordings of mutant mice deficient for the ortholog of the identified candidate gene, and performed immunohistochemistry using human and mouse brain specimens.ResultsAll affected individuals had ataxia, eye movement abnormalities, most notably tonic upgaze, and delayed speech and cognitive development. Homozygosity mapping identified the disease locus on chromosome 4q. Within this region, a homozygous deletion of GRID2 exon 4 in the index family and compound heterozygous deletions involving GRID2 exon 2 in the second family were identified. Grid2-deficient mice showed larger spontaneous and random eye movements compared to wild-type mice. In developing mouse and human cerebella, GRID2 localized to the Purkinje cell dendritic spines. Brain MRI in 2 affected children showed progressive cerebellar atrophy, which was more severe than that of Grid2-deficient mice.ConclusionsBiallelic deletions of GRID2 lead to a syndrome of cerebellar ataxia and tonic upgaze in humans. The phenotypic resemblance and similarity in protein expression pattern between humans and mice suggest a conserved role for GRID2 in the synapse organization between parallel fibers and Purkinje cells. However, the progressive and severe cerebellar atrophy seen in the affected individuals could indicate an evolutionarily unique role for GRID2 in the human cerebellum.

Published

2013

33. A genome-wide association study identifies susceptibility loci for nonsyndromic sagittal craniosynostosis near BMP2 and within BBS9

Author

Justice, Cristina M, Yagnik, Garima, Kim, Yoonhee, Peter, Inga, Jabs, Ethylin Wang, Erazo, Monica, Ye, Xiaoqian, Ainehsazan, Edmond, Shi, Lisong, Cunningham, Michael L, Kimonis, Virginia, Roscioli, Tony, Wall, Steven A, Wilkie, Andrew OM, Stoler, Joan, Richtsmeier, Joan T, Heuzé, Yann, Sanchez-Lara, Pedro A, Buckley, Michael F, Druschel, Charlotte M, Mills, James L, Caggana, Michele, Romitti, Paul A, Kay, Denise M, Senders, Craig, Taub, Peter J, Klein, Ophir D, Boggan, James, Zwienenberg-Lee, Marike, Naydenov, Cyrill, Kim, Jinoh, Wilson, Alexander F, and Boyadjiev, Simeon A

Subjects

Biological Sciences, Genetics, Human Genome, Rare Diseases, Bone Morphogenetic Protein 2, Cohort Studies, Craniosynostoses, Cytoskeletal Proteins, Genetic Loci, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Infant, Newborn, Male, Neoplasm Proteins, Oligonucleotide Array Sequence Analysis, Polymorphism, Single Nucleotide, Sex Factors, White People, Medical and Health Sciences, Developmental Biology, Agricultural biotechnology, Bioinformatics and computational biology

Abstract

Sagittal craniosynostosis is the most common form of craniosynostosis, affecting approximately one in 5,000 newborns. We conducted, to our knowledge, the first genome-wide association study for nonsyndromic sagittal craniosynostosis (sNSC) using 130 non-Hispanic case-parent trios of European ancestry (NHW). We found robust associations in a 120-kb region downstream of BMP2 flanked by rs1884302 (P = 1.13 × 10(-14), odds ratio (OR) = 4.58) and rs6140226 (P = 3.40 × 10(-11), OR = 0.24) and within a 167-kb region of BBS9 between rs10262453 (P = 1.61 × 10(-10), OR = 0.19) and rs17724206 (P = 1.50 × 10(-8), OR = 0.22). We replicated the associations to both loci (rs1884302, P = 4.39 × 10(-31) and rs10262453, P = 3.50 × 10(-14)) in an independent NHW population of 172 unrelated probands with sNSC and 548 controls. Both BMP2 and BBS9 are genes with roles in skeletal development that warrant functional studies to further understand the etiology of sNSC.

Published

2012

34. The Lower Anogenital Squamous Terminology Standardization Project for HPV-Associated Lesions: Background and Consensus Recommendations from the College of American Pathologists and the American Society for Colposcopy and Cervical Pathology

Author

Darragh, Teresa M, Colgan, Terence J, Cox, J Thomas, Heller, Debra S, Henry, Michael R, Luff, Ronald D, McCalmont, Timothy, Nayar, Ritu, Palefsky, Joel M, Stoler, Mark H, Wilkinson, Edward J, Zaino, Richard J, Wilbur, David C, O'Connor, Dennis M, Reynolds, R Kevin, Selim, M Angelica, Scurry, James, Chelmow, David, Howell, Lydia P, Ronnett, Brigitte, Waxman, Alan G, Haefner, Hope K, Leslie, Kieron S, Shea, Christopher, Staats, Paul N, Council, Leona, Lytwyn, Alice, Winkler, Barbara, Roberts, Jennifer, Downs, Levi, Laucirica, Rodolfo, Allbritton, Jill, Ioffe, Olga, Joste, Nancy, Berry, J Michael, Lin, Oscar, Welton, Mark, Otis, Christopher N, Bentz, Joel S, Kong, Christina S, Quade, Bradley, Schwartz, Mary R, Castle, Philip E, Duggan, Maire, Garcia, Francisco AR, Moriarty, Ann T, Niedt, G Chip, Carter, Alicia, Goodman, Marc, Neal, Margaret, Reddy, Vijaya, Robboy, Stanley, Saraiya, Mona, Silverberg, Steven, and Spires, Susan

Subjects

Sexually Transmitted Infections, Cervical Cancer, Infectious Diseases, Cancer, Female, Humans, Anus Neoplasms, Carcinoma in Situ, Genital Neoplasms, Female, Papillomavirus Infections, Terminology as Topic, Systematic Reviews as Topic, squamous intraepithelial lesion, human papillomavirus, superficially invasive carcinoma, p16, terminology, Members of LAST Project Work Groups, Clinical Sciences, Pathology

Abstract

The terminology for human papillomavirus(HPV)–associated squamous lesions of the lower anogenital tract has a long history marked by disparate diagnostic terms derived from multiple specialties. It often does not reflect current knowledge of HPV biology and pathogenesis. A consensus process was convened to recommend terminology unified across lower anogenital sites. The goal was to create a histopathologic nomenclature system that reflects current knowledge of HPV biology, optimally uses available biomarkers, and facilitates clear communication across different medical specialties. The Lower Anogenital Squamous Terminology (LAST) Project was co-sponsored by the College of American Pathologists and the American Society for Colposcopy and Cervical Pathology and included 5 working groups; 3 work groups performed comprehensive literature reviews and developed draft recommendations. Another work group provided the historical background and the fifth will continue to foster implementation of the LAST recommendations. After an open comment period, the draft recommendations were presented at a consensus conference attended by LAST work group members, advisors, and representatives from 35 stakeholder organizations including professional societies and government agencies. Recommendations were finalized and voted on at the consensus meeting. The final, approved recommendations standardize biologically relevant histopathologic terminology for HPV-associated squamous intraepithelial lesions and superficially invasive squamous carcinomas across all lower anogenital tract sites and detail the appropriate use of specific biomarkers to clarify histologic interpretations and enhance diagnostic accuracy. A plan for disseminating and monitoring recommendation implementation in the practicing community was also developed. The implemented recommendations will facilitate communication between pathologists and their clinical colleagues and improve accuracy of histologic diagnosis with the ultimate goal of providing optimal patient care.

Published

2012

35. The Lower Anogenital Squamous Terminology Standardization Project for HPV-Associated Lesions: background and consensus recommendations from the College of American Pathologists and the American Society for Colposcopy and Cervical Pathology.

Author

Darragh, Teresa M, Colgan, Terence J, Cox, J Thomas, Heller, Debra S, Henry, Michael R, Luff, Ronald D, McCalmont, Timothy, Nayar, Ritu, Palefsky, Joel M, Stoler, Mark H, Wilkinson, Edward J, Zaino, Richard J, Wilbur, David C, and Members of LAST Project Work Groups

Subjects

Members of LAST Project Work Groups, Humans, Papillomavirus Infections, Carcinoma in Situ, Anus Neoplasms, Genital Neoplasms, Female, Female, Terminology as Topic, squamous intraepithelial lesion, human papillomavirus, superficially invasive carcinoma, p16, terminology, Sexually Transmitted Infections, Cancer, Cervical Cancer, Infectious Diseases, Pathology, Clinical Sciences

Abstract

The terminology for human papillomavirus(HPV)–associated squamous lesions of the lower anogenital tract has a long history marked by disparate diagnostic terms derived from multiple specialties. It often does not reflect current knowledge of HPV biology and pathogenesis. A consensus process was convened to recommend terminology unified across lower anogenital sites. The goal was to create a histopathologic nomenclature system that reflects current knowledge of HPV biology, optimally uses available biomarkers, and facilitates clear communication across different medical specialties. The Lower Anogenital Squamous Terminology (LAST) Project was co-sponsored by the College of American Pathologists and the American Society for Colposcopy and Cervical Pathology and included 5 working groups; 3 work groups performed comprehensive literature reviews and developed draft recommendations. Another work group provided the historical background and the fifth will continue to foster implementation of the LAST recommendations. After an open comment period, the draft recommendations were presented at a consensus conference attended by LAST work group members, advisors, and representatives from 35 stakeholder organizations including professional societies and government agencies. Recommendations were finalized and voted on at the consensus meeting. The final, approved recommendations standardize biologically relevant histopathologic terminology for HPV-associated squamous intraepithelial lesions and superficially invasive squamous carcinomas across all lower anogenital tract sites and detail the appropriate use of specific biomarkers to clarify histologic interpretations and enhance diagnostic accuracy. A plan for disseminating and monitoring recommendation implementation in the practicing community was also developed. The implemented recommendations will facilitate communication between pathologists and their clinical colleagues and improve accuracy of histologic diagnosis with the ultimate goal of providing optimal patient care.

Published

2012

36. ALX4 gain-of-function mutations in non-syndromic craniosynostosis

Author

Yagnik, Garima, Ghuman, Apar, Kim, Sundon, Stevens, Cristina G., Kimonis, Virginia, Stoler, Joan, Sanchez-Lara, Pedro, Bernstein, Jonathan, Naydenov, Cyril, Drissi, Hicham, Cunningham, Michael L., Kim, Jinoh, and Boyadjiev, Simeon A.

Abstract

Craniosynostosis is the early fusion of one or more sutures of the infant skull and is a common defect occurring in approximately 1 of every 2,500 live births. Non-syndromic craniosynostosis accounts for approximately 80% of all cases and is thought to have strong genetic determinants that are yet to be identified. ALX4 is a homeodomain transcription factor with known involvement in osteoblast regulation. By direct sequencing of the ALX4 coding region in sagittal or sagittal-suture-involved non-syndromic craniosynostosis probands, we identified novel, nonsynonymous, familial variants in three of 203 individuals with NSC. Using dual-luciferase assay we show that two of these variants (V7F and K211E) confer a significant gain-of-function effect on ALX4. Our results suggest that ALX4 variants may have an impact on the genetic etiology of NSC.

Published

2012

37. The Lower Anogenital Squamous Terminology Standardization Project for HPV-Associated Lesions: background and consensus recommendations from the College of American Pathologists and the American Society for Colposcopy and Cervical Pathology.

Author

Darragh, Teresa M, Colgan, Terence J, Cox, J Thomas, Heller, Debra S, Henry, Michael R, Luff, Ronald D, McCalmont, Timothy, Nayar, Ritu, Palefsky, Joel M, Stoler, Mark H, Wilkinson, Edward J, Zaino, Richard J, Wilbur, David C, and Members of LAST Project Work Groups

Subjects

Members of LAST Project Work Groups, Vulva, Humans, Papillomavirus Infections, Carcinoma, Squamous Cell, Vaginal Neoplasms, Neoplasm Invasiveness, Precancerous Conditions, Colposcopy, Vaginal Smears, Neoplasm Staging, Reference Standards, Societies, Medical, United States, Anal Canal, Uterine Cervical Neoplasms, Female, Terminology as Topic, Practice Guidelines as Topic, Systematic Reviews as Topic, Cancer, Cervical Cancer, Infectious Diseases, Sexually Transmitted Infections, squamous intraepithelial lesion, human papillomavirus, superficially invasive carcinoma, p16, terminology, Clinical Sciences, Obstetrics & Reproductive Medicine

Abstract

The terminology for human papillomavirus (HPV)-associated squamous lesions of the lower anogenital tract has a long history marked by disparate diagnostic terms derived from multiple specialties. It often does not reflect current knowledge of HPV biology and pathogenesis. A consensus process was convened to recommend terminology unified across lower anogenital sites. The goal was to create a histopathologic nomenclature system that reflects current knowledge of HPV biology, optimally uses available biomarkers, and facilitates clear communication across different medical specialties. The Lower Anogenital Squamous Terminology (LAST) Project was cosponsored by the College of American Pathologists and the American Society for Colposcopy and Cervical Pathology and included 5 working groups; 3 work groups performed comprehensive literature reviews and developed draft recommendations. Another work group provided the historical background and the fifth will continue to foster implementation of the LAST recommendations. After an open comment period, the draft recommendations were presented at a consensus conference attended by LAST work group members, advisors, and representatives from 35 stakeholder organizations including professional societies and government agencies. Recommendations were finalized and voted on at the consensus meeting. The final, approved recommendations standardize biologically relevant histopathologic terminology for HPV-associated squamous intraepithelial lesions and superficially invasive squamous carcinomas across all lower anogenital tract sites and detail the appropriate use of specific biomarkers to clarify histologic interpretations and enhance diagnostic accuracy. A plan for disseminating and monitoring recommendation implementation in the practicing community was also developed. The implemented recommendations will facilitate communication between pathologists and their clinical colleagues and improve accuracy of histologic diagnosis with the ultimate goal of providing optimal patient care.

Published

2012

38. The Lower Anogenital Squamous Terminology Standardization Project for HPV-Associated Lesions: background and consensus recommendations from the College of American Pathologists and the American Society for Colposcopy and Cervical Pathology.

Author

Darragh, Teresa M, Colgan, Terence J, Cox, J Thomas, Heller, Debra S, Henry, Michael R, Luff, Ronald D, McCalmont, Timothy, Nayar, Ritu, Palefsky, Joel M, Stoler, Mark H, Wilkinson, Edward J, Zaino, Richard J, Wilbur, David C, and Members of LAST Project Work Groups

Subjects

Members of LAST Project Work Groups, Vulva, Humans, Papillomavirus Infections, Carcinoma, Squamous Cell, Vaginal Neoplasms, Neoplasm Invasiveness, Precancerous Conditions, Colposcopy, Vaginal Smears, Neoplasm Staging, Reference Standards, Societies, Medical, United States, Anal Canal, Uterine Cervical Neoplasms, Female, Terminology as Topic, Practice Guidelines as Topic, squamous intraepithelial lesion, human papillomavirus, superficially invasive carcinoma, p16, terminology, Cancer, Sexually Transmitted Infections, Cervical Cancer, Infectious Diseases, Obstetrics & Reproductive Medicine, Clinical Sciences

Abstract

The terminology for human papillomavirus (HPV)-associated squamous lesions of the lower anogenital tract has a long history marked by disparate diagnostic terms derived from multiple specialties. It often does not reflect current knowledge of HPV biology and pathogenesis. A consensus process was convened to recommend terminology unified across lower anogenital sites. The goal was to create a histopathologic nomenclature system that reflects current knowledge of HPV biology, optimally uses available biomarkers, and facilitates clear communication across different medical specialties. The Lower Anogenital Squamous Terminology (LAST) Project was cosponsored by the College of American Pathologists and the American Society for Colposcopy and Cervical Pathology and included 5 working groups; 3 work groups performed comprehensive literature reviews and developed draft recommendations. Another work group provided the historical background and the fifth will continue to foster implementation of the LAST recommendations. After an open comment period, the draft recommendations were presented at a consensus conference attended by LAST work group members, advisors, and representatives from 35 stakeholder organizations including professional societies and government agencies. Recommendations were finalized and voted on at the consensus meeting. The final, approved recommendations standardize biologically relevant histopathologic terminology for HPV-associated squamous intraepithelial lesions and superficially invasive squamous carcinomas across all lower anogenital tract sites and detail the appropriate use of specific biomarkers to clarify histologic interpretations and enhance diagnostic accuracy. A plan for disseminating and monitoring recommendation implementation in the practicing community was also developed. The implemented recommendations will facilitate communication between pathologists and their clinical colleagues and improve accuracy of histologic diagnosis with the ultimate goal of providing optimal patient care.

Published

2012

39. Deletions of NRXN1 (neurexin‐1) predispose to a wide spectrum of developmental disorders

Author

Ching, Michael SL, Shen, Yiping, Tan, Wen‐Hann, Jeste, Shafali S, Morrow, Eric M, Chen, Xiaoli, Mukaddes, Nahit M, Yoo, Seung‐Yun, Hanson, Ellen, Hundley, Rachel, Austin, Christina, Becker, Ronald E, Berry, Gerard T, Driscoll, Katherine, Engle, Elizabeth C, Friedman, Sandra, Gusella, James F, Hisama, Fuki M, Irons, Mira B, Lafiosca, Tina, LeClair, Elaine, Miller, David T, Neessen, Michael, Picker, Jonathan D, Rappaport, Leonard, Rooney, Cynthia M, Sarco, Dean P, Stoler, Joan M, Walsh, Christopher A, Wolff, Robert R, Zhang, Ting, Nasir, Ramzi H, Wu, Bai‐Lin, and Group, on behalf of the Children's Hospital Boston Genotype Phenotype Study

Subjects

Genetics, Intellectual and Developmental Disabilities (IDD), Pediatric, Autism, Brain Disorders, Mental Health, Aetiology, 2.1 Biological and endogenous factors, Mental health, Autistic Disorder, Child, Child Development Disorders, Pervasive, Comparative Genomic Hybridization, Developmental Disabilities, Female, Humans, Intellectual Disability, Language Development Disorders, Male, Mutation, Phenotype, Schizophrenia, Sequence Deletion, NRXN1, developmental disorders, array CGH, NRXN1 exonic deletions, CNV, Children's Hospital Boston Genotype Phenotype Study Group, Clinical Sciences, Neurosciences

Abstract

Research has implicated mutations in the gene for neurexin-1 (NRXN1) in a variety of conditions including autism, schizophrenia, and nicotine dependence. To our knowledge, there have been no published reports describing the breadth of the phenotype associated with mutations in NRXN1. We present a medical record review of subjects with deletions involving exonic sequences of NRXN1. We ascertained cases from 3,540 individuals referred clinically for comparative genomic hybridization testing from March 2007 to January 2009. Twelve subjects were identified with exonic deletions. The phenotype of individuals with NRXN1 deletion is variable and includes autism spectrum disorders, mental retardation, language delays, and hypotonia. There was a statistically significant increase in NRXN1 deletion in our clinical sample compared to control populations described in the literature (P = 8.9 x 10(-7)). Three additional subjects with NRXN1 deletions and autism were identified through the Homozygosity Mapping Collaborative for Autism, and this deletion segregated with the phenotype. Our study indicates that deletions of NRXN1 predispose to a wide spectrum of developmental disorders.

Published

2010

40. Deletions of NRXN1 (neurexin-1) predispose to a wide spectrum of developmental disorders.

Author

Ching, Michael SL, Shen, Yiping, Tan, Wen-Hann, Jeste, Shafali S, Morrow, Eric M, Chen, Xiaoli, Mukaddes, Nahit M, Yoo, Seung-Yun, Hanson, Ellen, Hundley, Rachel, Austin, Christina, Becker, Ronald E, Berry, Gerard T, Driscoll, Katherine, Engle, Elizabeth C, Friedman, Sandra, Gusella, James F, Hisama, Fuki M, Irons, Mira B, Lafiosca, Tina, LeClair, Elaine, Miller, David T, Neessen, Michael, Picker, Jonathan D, Rappaport, Leonard, Rooney, Cynthia M, Sarco, Dean P, Stoler, Joan M, Walsh, Christopher A, Wolff, Robert R, Zhang, Ting, Nasir, Ramzi H, Wu, Bai-Lin, and Children's Hospital Boston Genotype Phenotype Study Group

Subjects

Children's Hospital Boston Genotype Phenotype Study Group, Humans, Language Development Disorders, Child Development Disorders, Pervasive, Autistic Disorder, Developmental Disabilities, Schizophrenia, Sequence Deletion, Phenotype, Mutation, Child, Female, Male, Comparative Genomic Hybridization, Intellectual Disability, NRXN1, developmental disorders, array CGH, NRXN1 exonic deletions, CNV, Array CGH, Developmental disorders, Genetics, Clinical Sciences, Neurosciences

Abstract

Research has implicated mutations in the gene for neurexin-1 (NRXN1) in a variety of conditions including autism, schizophrenia, and nicotine dependence. To our knowledge, there have been no published reports describing the breadth of the phenotype associated with mutations in NRXN1. We present a medical record review of subjects with deletions involving exonic sequences of NRXN1. We ascertained cases from 3,540 individuals referred clinically for comparative genomic hybridization testing from March 2007 to January 2009. Twelve subjects were identified with exonic deletions. The phenotype of individuals with NRXN1 deletion is variable and includes autism spectrum disorders, mental retardation, language delays, and hypotonia. There was a statistically significant increase in NRXN1 deletion in our clinical sample compared to control populations described in the literature (P = 8.9 x 10(-7)). Three additional subjects with NRXN1 deletions and autism were identified through the Homozygosity Mapping Collaborative for Autism, and this deletion segregated with the phenotype. Our study indicates that deletions of NRXN1 predispose to a wide spectrum of developmental disorders.

Published

2010