Your search keyword '"Hildesheim A"' showing total 2,163 results

1. Differential long-term bivalent HPV vaccine cross-protection by variants in the Costa Rica HPV vaccine trial

Author

Shing, Jaimie Z., Porras, Carolina, Pinheiro, Maísa, Herrero, Rolando, Hildesheim, Allan, Liu, Danping, Gail, Mitchell H., Romero, Byron, Schiller, John T., Zúñiga, Michael, Mishra, Sambit, Burdette, Laurie, Jones, Kristine, Schussler, John, Ocampo, Rebeca, Fang, Jianwen, Liu, Zhiwei, Lowy, Douglas R., Tsang, Sabrina H., Rodríguez, Ana Cecilia, Schiffman, Mark, Haas, Cameron B., Carvajal, Loretto J., Brown, Jalen R., Kreimer, Aimée R., and Mirabello, Lisa

Published

2024

2. Evaluation of walking activity and gait to identify physical and mental fatigue in neurodegenerative and immune disorders: preliminary insights from the IDEA-FAST feasibility study

Author

Hinchliffe, Chloe, Rehman, Rana Zia Ur, Pinaud, Clemence, Branco, Diogo, Jackson, Dan, Ahmaniemi, Teemu, Guerreiro, Tiago, Chatterjee, Meenakshi, Manyakov, Nikolay V., Pandis, Ioannis, Davies, Kristen, Macrae, Victoria, Aufenberg, Svenja, Paulides, Emma, Hildesheim, Hanna, Kudelka, Jennifer, Emmert, Kirsten, Van Gassen, Geert, Rochester, Lynn, van der Woude, C. Janneke, Reilmann, Ralf, Maetzler, Walter, Ng, Wan-Fai, and Del Din, Silvia

Published

2024

3. COVID-19 and long-term impact on symptoms and Health-Related Quality of Life in Costa Rica: the RESPIRA cohort study

Author

Barboza-Solis, Cristina, Fantin, Romain, Hildesheim, Allan, Pfeiffer, Ruth, Porras, Carolina, Butt, Julia, Waterboer, Tim, Raventós, Henriette, Abdelnour, Arturo, Aparicio, Amada, Loria, Viviana, Prevots, D. Rebecca, Gail, Mitchell H., and Herrero, Rolando

Published

2024

4. The effects of repetitive transcranial magnetic stimulation on the brain of non-human primates with chronic stroke

Author

Adan-Ulises Dominguez-Vargas, Proulx Camille, Adarsh Kumar, Franziska Hildesheim, Stephan Quessy, Alexander Thiel, Douglas Cook, Stephen Scott, and Numa Dancause

Subjects

Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Published

2025

5. A surveillance study of cancer incidence and mortality among young adults in Costa Rica

Author

Slimovitch, Rachel, Shing, Jaimie Z., Fantin, Romain, Vanegas, Juan C., Porras, Carolina, Herrero, Rolando, Shiels, Meredith S., Sierra, Mónica S., Stephens, Erica S., Hildesheim, Allan, Kreimer, Aimée R., Calderón, Alejandro, and Carvajal, Loretto J.

Published

2024

6. 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

7. Precancerous cervical lesions caused by non-vaccine-preventable HPV types after vaccination with the bivalent AS04-adjuvanted HPV vaccine: an analysis of the long-term follow-up study from the randomised Costa Rica HPV Vaccine Trial.

Author

Shing, Jaimie, Hu, Shangying, Herrero, Rolando, Hildesheim, Allan, Porras, Carolina, Sampson, Joshua, Schussler, John, Schiller, John, Lowy, Douglas, Sierra, Mónica, Carvajal, Loretto, and Kreimer, Aimée

Subjects

Adolescent, Adult, Costa Rica, Female, Follow-Up Studies, Human papillomavirus 16, Human papillomavirus 18, Humans, Male, Papillomaviridae, Papillomavirus Infections, Papillomavirus Vaccines, Precancerous Conditions, Uterine Cervical Neoplasms, Vaccination, Young Adult, Uterine Cervical Dysplasia

Abstract

BACKGROUND: In women vaccinated against human papillomavirus (HPV), reductions in cervical disease and related procedures results in more women having intact transformation zones, potentially increasing the risk of cervical lesions caused by non-vaccine-preventable HPV types, a phenomenon termed clinical unmasking. We aimed to evaluate HPV vaccine efficacy against cervical intraepithelial neoplasia grade 2 or worse (CIN2+) and cervical intraepithelial neoplasia grade 3 or worse (CIN3+) attributed to non-preventable HPV types in the long-term follow-up phase of the Costa Rica HPV Vaccine Trial (CVT). METHODS: CVT was a randomised, double-blind, community-based trial done in Costa Rica. Eligible participants were women aged 18-25 years who were in general good health. Participants were randomly assigned (1:1) to receive an HPV 16 and 18 AS04-adjuvanted vaccine or control hepatitis A vaccine, using a blocked randomisation method (permuted block sizes of 14, 16, and 18). Vaccines in both groups were administered intramuscularly with 0·5 mL doses at 0, 1, and 6 months. Masking of vaccine allocation was maintained throughout the 4-year randomised trial phase, after which participants in the hepatitis A virus vaccine control group were provided the HPV vaccine and exited the study; a screening-only, unvaccinated control group was enrolled. The unvaccinated control group and HPV vaccine group were followed up for 7 years, during which treatment allocation was not masked. One of the prespecified primary endpoints for the long-term follow-up phase was precancers associated with HPV types not prevented by the vaccine, defined as histologically confirmed incident CIN2+ events or CIN3+ events attributed to any HPV type except HPV 16, 18, 31, 33, and 45. Our primary analytical period was years 7-11. Primary analyses were in all participants with at least one follow-up visit and excluded participants with a previous endpoint (ie, modified intention-to-treat cohort). Safety endpoints have been reported elsewhere. This trial is registered with ClinicalTrials.gov, NCT00128661 and NCT00867464. The randomised, masked trial phase is completed; an unmasked subset of women in the HPV-vaccinated group is under active investigation. FINDINGS: Between June 28, 2004, and Dec 21, 2005, 7466 participants were enrolled (HPV vaccine group n=3727 and hepatitis A virus vaccine control group n=3739). Between March 30, 2009, and July 5, 2012, 2836 women enrolled in the new unvaccinated control group. The primary analytical cohort (years 7 to 11) included 2767 participants in the HPV vaccine group and 2563 in the unvaccinated group for the CIN2+ events endpoint assessment and 2826 participants in the HPV vaccine group and 2592 in the unvaccinated control group for the CIN3+ events endpoint assessment. Median follow-up during years 7 to 11 for women included for the CIN2+ events analysis was 52·8 months (IQR 44·0 to 60·7) for the HPV vaccine group and 49·8 months (42·0 to 56·9) for the unvaccinated control group. During years 7 to 11, clinical unmasking was observed with a negative vaccine efficacy against CIN2+ events attributed to non-preventable HPV types (-71·2% [95% CI -164·0 to -12·5]), with 9·2 (95% CI 2·1 to 15·6) additional CIN2+ events attributed to non-preventable HPV types per 1000 HPV-vaccinated participants versus HPV-unvaccinated participants. 27·0 (95% CI 14·2 to 39·9) fewer CIN2+ events irrespective of HPV type per 1000 vaccinated participants were observed during 11 years of follow-up. Vaccine efficacy against CIN3+ events attributed to non-preventable HPV types during years 7 to 11 was -135·0% (95% CI -329·8 to -33·5), with 8·3 (3·0 to 12·8) additional CIN3+ events attributed to non-preventable HPV types per 1000 vaccinated participants versus unvaccinated participants. INTERPRETATION: Higher rates of CIN2+ events and CIN3+ events due to non-preventable HPV types in vaccinated versus unvaccinated participants suggests clinical unmasking could attenuate long-term reductions in high-grade disease following successful implementation of HPV vaccination programmes in screened populations. Importantly, the net benefit of vaccination remains considerable; therefore, HPV vaccination should still be prioritised as primary prevention for cervical cancer. FUNDING: National Cancer Institute and National Institutes of Health Office of Research on Womens Health. TRANSLATION: For the Spanish translation of the abstract see Supplementary Materials section.

Published

2022

8. Fatigue-Related Changes of Daily Function: Most Promising Measures for the Digital Age

Author

Walter Maetzler, Leonor Correia Guedes, Kirsten Nele Emmert, Jennifer Kudelka, Hanna Luise Hildesheim, Emma Paulides, Hayley Connolly, Kristen Davies, Valentina Dilda, Teemu Ahmaniemi, Luisa Avedano, Raquel Bouça-Machado, Michael Chambers, Meenakshi Chatterjee, Peter Gallagher, Johanna Graeber, Corina Maetzler, Hanna Kaduszkiewicz, Norelee Kennedy, Victoria Macrae, Laura Carrasco Marín, Anusha Moses, Alessandro Padovani, Andrea Pilotto, Natasha Ratcliffe, Ralf Reilmann, Madalena Rosario, Stefan Schreiber, Dina De Sousa, Geert Van Gassen, Lori Ann Warring, Klaus Seppi, C. Janneke van der Woude, Joaquim J. Ferreira, and Wan-Fai Ng

Subjects

activities of daily life, international classification of functioning, disability and health, performance, wearables, Biology (General), QH301-705.5

Abstract

Background: Fatigue is a prominent symptom in many diseases and is strongly associated with impaired daily function. The measurement of daily function is currently almost always done with questionnaires, which are subjective and imprecise. With the recent advances of digital wearable technologies, novel approaches to evaluate daily function quantitatively and objectively in real-life conditions are increasingly possible. This also creates new possibilities to measure fatigue-related changes of daily function using such technologies. Summary: This review examines which digitally assessable parameters in immune-mediated inflammatory and neurodegenerative diseases may have the greatest potential to reflect fatigue-related changes of daily function. Key Messages: Results of a standardized analysis of the literature reporting about perception-, capacity-, and performance-evaluating assessment tools indicate that changes of the following parameters: physical activity, independence of daily living, social participation, working life, mental status, cognitive and aerobic capacity, and supervised and unsupervised mobility performance have the highest potential to reflect fatigue-related changes of daily function. These parameters thus hold the greatest potential for quantitatively measuring fatigue in representative diseases in real-life conditions, e.g., with digital wearable technologies. Furthermore, to the best of our knowledge, this is a new approach to analysing evidence for the design of performance-based digital assessment protocols in human research, which may stimulate further systematic research in this area.

Published

2024

9. SARS-CoV-2 infection prior to vaccination amplifies Fc-mediated humoral profiles in an age-dependent manner

Author

Jung, Wonyeong, Abdelnour, Arturo, Kaplonek, Paulina, Herrero, Rolando, Shih-Lu Lee, Jessica, Barbati, Domenic R., Chicz, Taras M., Levine, Kate S., Fantin, Romain Clement, Loria, Viviana, Porras, Carolina, Lauffenburger, Douglas A., Gail, Mitchell H., Aparicio, Amada, Hildesheim, Allan, Alter, Galit, and McNamara, Ryan P.

Published

2024

10. HPV16 infection decreases vaccine-induced HPV16 antibody avidity: the CVT trial.

Author

Tsang, Sabrina, Schiller, John, Porras, Carolina, Kemp, Troy, Herrero, Rolando, Schussler, John, Sierra, Monica, Cortes, Bernal, Hildesheim, Allan, Lowy, Douglas, Rodríguez, Ana, Romero, Byron, Çuburu, Nicolas, Shing, Jaimie, Pinto, Ligia, Sampson, Joshua, and Kreimer, Aimée

Abstract

The HPV vaccine has shown sustained efficacy and consistent stabilization of antibody levels, even after a single dose. We defined the HPV16-VLP antibody avidity patterns over 11 years among women who received one- or three doses of the bivalent HPV vaccine in the Costa Rica HPV Vaccine Trial. Absolute HPV16 avidity was lower in women who received one compared to three doses, although the patterns were similar (increased in years 2 and 3 and remained stable over the remaining 8 years). HPV16 avidity among women who were HPV16-seropositive women at HPV vaccination, a marker of natural immune response to HPV16 infection, was significantly lower than those of HPV16-seronegative women, a difference that was more pronounced among one-dose recipients. No differences in HPV16 avidity were observed by HPV18 serostatus at vaccination, confirming the specificity of the findings. Importantly, point estimates for vaccine efficacy against incident, six-month persistent HPV16 infections was similar between women who were HPV16 seronegative and seropositive at the time of initial HPV vaccination for both one-dose and three-dose participants. It is therefore likely that this lower avidity level is still sufficient to enable antibody-mediated protection. It is encouraging for long-term HPV-vaccine protection that HPV16 antibody avidity was maintained for over a decade, even after a single dose.

Published

2022

11. Therapy-Induced Senescence: Opportunities to Improve Anticancer Therapy.

Author

Prasanna, Pataje G, Citrin, Deborah E, Hildesheim, Jeffrey, Ahmed, Mansoor M, Venkatachalam, Sundar, Riscuta, Gabriela, Xi, Dan, Zheng, Guangrong, Deursen, Jan van, Goronzy, Jorg, Kron, Stephen J, Anscher, Mitchell S, Sharpless, Norman E, Campisi, Judith, Brown, Stephen L, Niedernhofer, Laura J, O'Loghlen, Ana, Georgakilas, Alexandros G, Paris, Francois, Gius, David, Gewirtz, David A, Schmitt, Clemens A, Abazeed, Mohamed E, Kirkland, James L, Richmond, Ann, Romesser, Paul B, Lowe, Scott W, Gil, Jesus, Mendonca, Marc S, Burma, Sandeep, Zhou, Daohong, and Coleman, C Norman

Subjects

Cancer, Prevention, Oncology & Carcinogenesis, Oncology and Carcinogenesis

Abstract

Cellular senescence is an essential tumor suppressive mechanism that prevents the propagation of oncogenically activated, genetically unstable, and/or damaged cells. Induction of tumor cell senescence is also one of the underlying mechanisms by which cancer therapies exert antitumor activity. However, an increasing body of evidence from preclinical studies demonstrates that radiation and chemotherapy cause accumulation of senescent cells (SnCs) both in tumor and normal tissue. SnCs in tumors can, paradoxically, promote tumor relapse, metastasis, and resistance to therapy, in part, through expression of the senescence-associated secretory phenotype. In addition, SnCs in normal tissue can contribute to certain radiation- and chemotherapy-induced side effects. Because of its multiple roles, cellular senescence could serve as an important target in the fight against cancer. This commentary provides a summary of the discussion at the National Cancer Institute Workshop on Radiation, Senescence, and Cancer (August 10-11, 2020, National Cancer Institute, Bethesda, MD) regarding the current status of senescence research, heterogeneity of therapy-induced senescence, current status of senotherapeutics and molecular biomarkers, a concept of "one-two punch" cancer therapy (consisting of therapeutics to induce tumor cell senescence followed by selective clearance of SnCs), and its integration with personalized adaptive tumor therapy. It also identifies key knowledge gaps and outlines future directions in this emerging field to improve treatment outcomes for cancer patients.

Published

2021

12. Therapy-Induced Senescence: Opportunities to Improve Anti-Cancer Therapy

Author

Prasanna, Pataje G, Citrin, Deborah E, Hildesheim, Jeffrey, Ahmed, Mansoor M, Venkatachalam, Sundar, Riscuta, Gabriela, Xi, Dan, Zheng, Guangrong, van Deursen, Jan, Goronzy, Jorg, Kron, Stephen J, Anscher, Mitchell S, Sharpless, Norman E, Campisi, Judith, Brown, Stephen L, Niedernhofer, Laura J, O'Loghlen, Ana, Georgakilas, Alexandros G, Paris, Francois, Gius, David, Gewirtz, David A, Schmitt, Clemens A, Abazeed, Mohamed E, Kirkland, James L, Richmond, Ann, Romesser, Paul B, Lowe, Scott W, Gil, Jesus, Mendonca, Marc S, Burma, Sandeep, Zhou, Daohong, and Coleman, C Norman

Subjects

Cancer, Prevention, Good Health and Well Being, Biomarkers, Cellular Senescence, Humans, Neoplasms, Senescence-Associated Secretory Phenotype, Oncology and Carcinogenesis, Oncology & Carcinogenesis

Abstract

Cellular senescence is an essential tumor suppressive mechanism that prevents the propagation of oncogenically activated, genetically unstable, and/or damaged cells. Induction of tumor cell senescence is also one of the underlying mechanisms by which cancer therapies exert antitumor activity. However, an increasing body of evidence from preclinical studies demonstrates that radiation and chemotherapy cause accumulation of senescent cells (SnCs) both in tumor and normal tissue. SnCs in tumors can, paradoxically, promote tumor relapse, metastasis, and resistance to therapy, in part, through expression of the senescence-associated secretory phenotype. In addition, SnCs in normal tissue can contribute to certain radiation- and chemotherapy-induced side effects. Because of its multiple roles, cellular senescence could serve as an important target in the fight against cancer. This commentary provides a summary of the discussion at the National Cancer Institute Workshop on Radiation, Senescence, and Cancer (August 10-11, 2020, National Cancer Institute, Bethesda, MD) regarding the current status of senescence research, heterogeneity of therapy-induced senescence, current status of senotherapeutics and molecular biomarkers, a concept of "one-two punch" cancer therapy (consisting of therapeutics to induce tumor cell senescence followed by selective clearance of SnCs), and its integration with personalized adaptive tumor therapy. It also identifies key knowledge gaps and outlines future directions in this emerging field to improve treatment outcomes for cancer patients.

Published

2021

13. A large, population-based study of age-related associations between vaginal pH and human papillomavirus infection

Author

Clarke Megan A, Rodriguez Ana, Gage Julia C, Herrero Rolando, Hildesheim Allan, Wacholder Sholom, Burk Robert, and Schiffman Mark

Subjects

HPV, Vaginal pH, Cervical neoplasia, Aging, Chlamydia, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background Vaginal pH is related to genital tract inflammation and changes in the bacterial flora, both suggested cofactors for persistence of human papillomavirus (HPV) infection. To evaluate the relationship between vaginal pH and HPV, we analyzed data from our large population-based study in Guanacaste, Costa Rica. We examined vaginal pH and the risk of HPV infection, cytological abnormalities, and C. trachomatis infection. Methods Our study included 9,165 women aged 18-97 at enrollment with a total of 28,915 visits (mean length of follow-up = 3.4 years). Generalized estimating equations were used to evaluate the relationship between vaginal pH and HPV infection (both overall and single versus multiple types) and low-grade squamous intraepithelial lesions (LSIL), the cytomorphic manifestation of HPV infection. The relationship between enrollment vaginal pH and C. trachomatis infection was assessed by logistic regression. Results were stratified by age at visit. Results Detection of HPV was positively associated with vaginal pH, mainly in women < 35 years (p-trend = 0.009 and 0.007 for women aged < 25 and 25-34 years, respectively). Elevated vaginal pH was associated with 30% greater risk of infection with multiple HPV types and with LSIL, predominantly in women younger than 35 and 65+ years of age. Detection of C. trachomatis DNA was associated with increased vaginal pH in women < 25 years (OR 2.2 95% CI 1.0-5.0). Conclusions Our findings suggest a possible association of the cervical microenvironment as a modifier of HPV natural history in the development of cervical precancer and cancer. Future research should include studies of vaginal pH in a more complex assessment of hormonal changes and the cervicovaginal microbiome as they relate to the natural history of cervical neoplasia.

Published

2012

14. 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

15. Determinants of seropositivity among HPV-16/18 DNA positive young women

Author

Porras Carolina, Bennett Christina, Safaeian Mahboobeh, Coseo Sarah, Rodríguez Ana Cecilia, González Paula, Hutchinson Martha, Jiménez Silvia, Sherman Mark E, Wacholder Sholom, Solomon Diane, van Doorn Leen-Jan, Bougelet Catherine, Quint Wim, Schiffman Mark, Herrero Rolando, and Hildesheim Allan

Subjects

Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background Not all women infected with HPV-16/18 have detectable levels of HPV-16/18 antibodies, those who seroconvert develop low antibody levels, and seroconversion occurs typically several months post-infection. We evaluated determinants of seropositivity among 646 women infected with HPV-16 and/or HPV-18. Methods Data are from the enrollment visit of the NCI-sponsored Costa Rica HPV Vaccine Trial. Sera were tested for HPV-16/18 antibodies by ELISA; cervical specimens were tested for HPV DNA using HC2 and SPF10/LiPA25. Odds ratios (OR) and 95% confidence intervals (CI) were computed. Results Among HPV-16/18 DNA positives, seropositivity was 63.0% and 57.5%, respectively. Among HPV-16 DNA positives, seropositivity increased with lifetime number of sexual partners (p-trend = 0.01). Women with abnormal cytology and/or high viral load had a 1.63-2.79-fold increase in the detection of antibodies compared to women with normal cytology/low viral load. Current users of oral contraceptives had a 1.88-fold (95%CI, 1.14-3.09) increased detection of antibodies and current users of injectables had a 3.38-fold (95%CI, 1.39-8.23) increased detection compared to never users. Among HPV-18 DNA positive women, seropositivity was associated with current oral contraceptive use (OR 2.47; 95%CI 1.08-5.65). Conclusions Factors associated with sustained HPV exposure (abnormal cytology, elevated HPV viral load, increasing lifetime partners) were predictive of HPV-16 seropositivity. Hormonal contraceptive use was associated with seropositivity suggesting an effect of hormones on immune responses to HPV. Patterns were less consistent for HPV-18. Follow up of incident HPV infections to evaluate seroconversion and their determinants is needed.

Published

2010

16. Remibrutinib (LOU064) inhibits neuroinflammation driven by B cells and myeloid cells in preclinical models of multiple sclerosis

Author

Barbara Nuesslein-Hildesheim, Enrico Ferrero, Cindy Schmid, Catherine Huck, Paul Smith, Sarah Tisserand, Joelle Rubert, Frederic Bornancin, Denis Eichlisberger, and Bruno Cenni

Subjects

Multiple sclerosis, BTK, Remibrutinib, LOU064, Autoimmunity, Neuroinflammation, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background Bruton’s tyrosine kinase (BTK) is a key signaling node in B cell receptor (BCR) and Fc receptor (FcR) signaling. BTK inhibitors (BTKi) are an emerging oral treatment option for patients suffering from multiple sclerosis (MS). Remibrutinib (LOU064) is a potent, highly selective covalent BTKi with a promising preclinical and clinical profile for MS and other autoimmune or autoallergic indications. Methods The efficacy and mechanism of action of remibrutinib was assessed in two different experimental autoimmune encephalomyelitis (EAE) mouse models for MS. The impact of remibrutinib on B cell-driven EAE pathology was determined after immunization with human myelin oligodendrocyte glycoprotein (HuMOG). The efficacy on myeloid cell and microglia driven neuroinflammation was determined in the RatMOG EAE. In addition, we assessed the relationship of efficacy to BTK occupancy in tissue, ex vivo T cell response, as well as single cell RNA-sequencing (scRNA-seq) in brain and spinal cord tissue. Results Remibrutinib inhibited B cell-dependent HuMOG EAE in dose-dependent manner and strongly reduced neurological symptoms. At the efficacious oral dose of 30 mg/kg, remibrutinib showed strong BTK occupancy in the peripheral immune organs and in the brain of EAE mice. Ex vivo MOG-specific T cell recall response was reduced, but not polyclonal T cell response, indicating absence of non-specific T cell inhibition. Remibrutinib also inhibited RatMOG EAE, suggesting that myeloid cell and microglia inhibition contribute to its efficacy in EAE. Remibrutinib did not reduce B cells, total Ig levels nor MOG-specific antibody response. In brain and spinal cord tissue a clear anti-inflammatory effect in microglia was detected by scRNA-seq. Finally, remibrutinib showed potent inhibition of in vitro immune complex-driven inflammatory response in human microglia. Conclusion Remibrutinib inhibited EAE models by a two-pronged mechanism based on inhibition of pathogenic B cell autoreactivity, as well as direct anti-inflammatory effects in microglia. Remibrutinib showed efficacy in both models in absence of direct B cell depletion, broad T cell inhibition or reduction of total Ig levels. These findings support the view that remibrutinib may represent a novel treatment option for patients with MS.

Published

2023

17. Statin use is not associated with inflammation among Chilean women of Mapuche and non-Mapuche ancestry with gallstones

Author

Sarah S Jackson, Marina Lex, Vanessa Van De Wyngard, Paz Cook, Allan Hildesheim, Ligia A Pinto, Sharon H Jackson, Kelvin Choi, Tsion Zewdu Minas, Héctor Fabio Losada Morales, Juan Carlos Araya, Catterina Ferreccio, Jill Koshiol, and Ruth M Pfeiffer

Subjects

Chile, gallstones, inflammation, Mapuche, statins, women, Medicine, Medicine (General), R5-920

Abstract

Aim: Statins are associated with lower risk of gallstones due to anti-inflammatory effects. We assessed whether statins impact circulating inflammation among Chilean women with gallstones. Materials & methods: 200 Mapuche women were matched on statin use and age to 200 non-Mapuche women in the Chile Biliary Longitudinal Study. We analyzed 92 inflammatory biomarkers using multivariable-adjusted regression models, random forests and pathway analyses. Results: Statins were not significantly associated with any inflammation marker when women were analyzed jointly or stratified by ancestry. No significant associations were found through random forest methods and pathway analyses. Discussion: We did not find significant associations between statin use and inflammation markers in women with gallstones, suggesting that statins do not reduce inflammation once gallstones have formed.

Published

2024

18. Estimating the cumulative incidence of SARS-CoV-2 infection in Costa Rica: modelling seroprevalence data in a population-based cohort

Author

Calderón, Alejandro, Moreno, Karla, Morera, Melvin, Wong, Roy, Castro, Roberto, Cortés, Bernal, Ocampo, Rebecca, Zúñiga, Michael, Vanegas, Juan Carlos, Sun, Kaiyuan, Barboza-Solís, Cristina, Binder, Marco, Fantin, Romain, Agarwala, Neha, Aparicio, Amada, Pfeiffer, Ruth, Waterboer, Tim, Abdelnour, Arturo, Butt, Julia, Flock, Julia, Remans, Kim, Prevots, D. Rebecca, Porras, Carolina, Hildesheim, Allan, Loria, Viviana, Gail, Mitchell H., and Herrero, Rolando

Published

2023

19. Behavioral factors and SARS-CoV-2 transmission heterogeneity within a household cohort in Costa Rica

Author

Sun, Kaiyuan, Loria, Viviana, Aparicio, Amada, Porras, Carolina, Vanegas, Juan Carlos, Zúñiga, Michael, Morera, Melvin, Avila, Carlos, Abdelnour, Arturo, Gail, Mitchell H., Pfeiffer, Ruth, Cohen, Jeffrey I., Burbelo, Peter D., Abed, Mehdi A., Viboud, Cécile, Hildesheim, Allan, Herrero, Rolando, and Prevots, D. Rebecca

Published

2023

20. 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

21. Evaluation of Durability of a Single Dose of the Bivalent HPV Vaccine: The CVT Trial.

Author

Kreimer, Aimée, Sampson, Joshua, Porras, Carolina, Schiller, John, Kemp, Troy, Herrero, Rolando, Wagner, Sarah, Boland, Joseph, Schussler, John, Lowy, Douglas, Chanock, Stephen, Roberson, David, Sierra, Mónica, Tsang, Sabrina, Schiffman, Mark, Rodriguez, Ana, Cortes, Bernal, Gail, Mitchell, Hildesheim, Allan, Gonzalez, Paula, and Pinto, Ligia

Subjects

Adolescent, Adult, Antibodies, Viral, Costa Rica, Female, Human papillomavirus 16, Human papillomavirus 18, Humans, Papillomavirus Infections, Papillomavirus Vaccines, Vaccines, Combined, Young Adult

Abstract

BACKGROUND: The authors investigated the durability of vaccine efficacy (VE) against human papillomavirus (HPV)16 or 18 infections and antibody response among nonrandomly assigned women who received a single dose of the bivalent HPV vaccine compared with women who received multiple doses and unvaccinated women. METHODS: HPV infections were compared between HPV16 or 18-vaccinated women aged 18 to 25 years who received one (N = 112), two (N = 62), or three (N = 1365) doses, and age- and geography-matched unvaccinated women (N = 1783) in the long-term follow-up of the Costa Rica HPV Vaccine Trial. Cervical HPV infections were measured at two study visits, approximately 9 and 11 years after initial HPV vaccination, using National Cancer Institute next-generation sequencing TypeSeq1 assay. VE and 95% confidence intervals (CIs) were estimated. HPV16 or 18 antibody levels were measured in all one- and two-dose women, and a subset of three-dose women, using a virus-like particle-based enzyme-linked immunosorbent assay (n = 448). RESULTS: Median follow-up for the HPV-vaccinated group was 11.3 years (interquartile range = 10.9-11.7 years) and did not vary by dose group. VE against prevalent HPV16 or 18 infection was 80.2% (95% CI = 70.7% to 87.0%) among three-dose, 83.8% (95% CI = 19.5% to 99.2%) among two-dose, and 82.1% (95% CI = 40.2% to 97.0%) among single-dose women. HPV16 or 18 antibody levels did not qualitatively decline between years four and 11 regardless of the number of doses given, although one-dose titers continue to be statistically significantly lower compared with two- and three-dose titers. CONCLUSION: More than a decade after HPV vaccination, single-dose VE against HPV16 or 18 infection remained high and HPV16 or 18 antibodies remained stable. A single dose of bivalent HPV vaccine may induce sufficiently durable protection that obviates the need for more doses.

Published

2020

22. Durability of Cross-Protection by Different Schedules of the Bivalent HPV Vaccine: The CVT Trial.

Author

Tsang, Sabrina, Sampson, Joshua, Schussler, John, Porras, Carolina, Wagner, Sarah, Boland, Joseph, Cortes, Bernal, Lowy, Douglas, Schiller, John, Schiffman, Mark, Kemp, Troy, Rodriguez, Ana, Quint, Wim, Gail, Mitchell, Pinto, Ligia, Gonzalez, Paula, Hildesheim, Allan, Kreimer, Aimée, and Herrero, Rolando

Subjects

Adolescent, Adult, Alphapapillomavirus, Cohort Studies, Costa Rica, Cross Protection, Female, Human papillomavirus 31, Humans, Immunization Schedule, Papillomavirus Infections, Papillomavirus Vaccines, Prevalence, Vaccines, Combined, Young Adult

Abstract

BACKGROUND: The Costa Rica HPV Vaccine Trial has documented cross-protection of the bivalent HPV vaccine against HPV31/33/45 up to 7 years after vaccination, even with one dose of the vaccine. However, the durability of such protection remains unknown. Here, we evaluate the efficacy of different schedules of the vaccine against HPV31/33/45 out to 11 years postvaccination, expanding to other nontargeted HPV types. METHODS: We compared the rates of HPV infection in vaccinated women with the rates in a comparable cohort of unvaccinated women. We estimated the average vaccine efficacy (VEavg) against incident infections and tested for a change in VE over time. RESULTS: Among 3-dose women, we observed statistically significant cross-protection against HPV31/33/45 (VEavg = 64.4%, 95% confidence interval [CI] = 57.7% to 70.0%). Additionally, we observed borderline, statistically significant cross-protection against HPV35 (VEavg = 23.2%, 95% CI = 0.3% to 40.8%) and HPV58 (VEavg = 21.2%, 95% CI = 4.2% to 35.3%). There was no decrease in VE over time (two-sided Ptrend > .05 for HPV31, -33, -35, -45, and -58). As a benchmark, VEavg against HPV16/18 was 82.0% (95% CI = 77.3% to 85.7%). Among 1-dose women, we observed comparable efficacy against HPV31/33/45 (VEavg = 54.4%, 95% CI = 21.0% to 73.7%). Acquisition of nonprotected HPV types was similar between vaccinated and unvaccinated women, indicating that the difference in HPV infection rates was not attributable to differential genital HPV exposure. CONCLUSIONS: Substantial cross-protection afforded by the bivalent vaccine against HPV31/33/45, and to a lesser extent, HPV35 and HPV58, was sustained and remained stable after 11 years postvaccination, reinforcing the notion that the bivalent vaccine is an effective option for protection against HPV-associated cancers.

Published

2020

23. Efficacy of the AS04-Adjuvanted HPV16/18 Vaccine: Pooled Analysis of the Costa Rica Vaccine and PATRICIA Randomized Controlled Trials.

Author

Tota, Joseph, Struyf, Frank, Sampson, Joshua, Gonzalez, Paula, Ryser, Martin, Herrero, Rolando, Schussler, John, Karkada, Naveen, Rodriguez, Ana, Folschweiller, Nicolas, Porras, Carolina, Schiffman, Mark, Schiller, John, Quint, Wim, Kreimer, Aimée, Wheeler, Cosette, and Hildesheim, Allan

Subjects

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

Abstract

BACKGROUND: The 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 . METHODS: Data 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. RESULTS: A 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

24. 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

25. Excess mortality from COVID 19 in Costa Rica: a registry based study using Poisson regression

Author

Fantin, Romain, Barboza-Solís, Cristina, Hildesheim, Allan, and Herrero, Rolando

Published

2023

26. Cohort profile: evaluation of immune response and household transmission of SARS-CoV-2 in Costa Rica: the RESPIRA study

Author

Allan Hildesheim, Tim Waterboer, Julia Butt, Mitchell H Gail, Alejandro Calderón, Rolando Herrero, Carolina Porras, Bernal Cortes, Viviana Loría, Amada Aparicio, Gloriana Barrientos, Daniela Retana, Kaiyuan Sun, Rebeca Ocampo, D. Rebecca Prevots, Michael Zúñiga, Roy Wong-McClure, Melvin Morera, Marco Binder, Arturo Abdelnour, Ruth M Pfeiffer, Cristina Barboza Solís, Romain Fantin, Juan Carlos Vanegas, Rachel Mercado, and Carlos Ávila

Subjects

Medicine

Abstract

Purpose The RESPIRA cohort aims to describe the nature, magnitude, time course and efficacy of the immune response to SARS-CoV-2 infection and vaccination, population prevalence, and household transmission of COVID-19.Participants From November 2020, we selected age-stratified random samples of COVID-19 cases from Costa Rica confirmed by PCR. For each case, two population-based controls, matched on age, sex and census tract were recruited, supplemented with hospitalised cases and household contacts. Participants were interviewed and blood and saliva collected for antibodies and PCR tests. Participants will be followed for 2 years to assess antibody response and infection incidence.Findings to date Recruitment included 3860 individuals: 1150 COVID-19 cases, 1999 population controls and 719 household contacts from 304 index cases. The age and regional distribution of cases was as planned, including four age strata, 30% rural and 70% urban. The control cohort had similar sex, age and regional distribution as the cases according to the study design. Among the 1999 controls recruited, 6.8% reported at enrolment having had COVID-19 and an additional 12.5% had antibodies against SARS-CoV-2. Compliance with visits and specimens has been close to 70% during the first 18 months of follow-up. During the study, national vaccination was implemented and nearly 90% of our cohort participants were vaccinated during follow-up.Future plans RESPIRA will enable multiple analyses, including population prevalence of infection, clinical, behavioural, immunological and genetic risk factors for SARS-CoV-2 acquisition and severity, and determinants of household transmission. We are conducting retrospective and prospective assessment of antibody levels, their determinants and their protective efficacy after infection and vaccination, the impact of long-COVID and a series of ancillary studies. Follow-up continues with bimonthly saliva collection for PCR testing and biannual blood collection for immune response analyses. Follow-up will be completed in early 2024.Trial registration number NCT04537338.

Published

2023

27. 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

28. Fatigue and cognitive impairment after COVID-19: A prospective multicentre study

Author

Hartung, Tim J., Neumann, Christian, Bahmer, Thomas, Chaplinskaya-Sobol, Irina, Endres, Matthias, Geritz, Johanna, Haeusler, Karl Georg, Heuschmann, Peter U., Hildesheim, Hanna, Hinz, Andreas, Hopff, Sina, Horn, Anna, Krawczak, Michael, Krist, Lilian, Kudelka, Jennifer, Lieb, Wolfgang, Maetzler, Corina, Mehnert-Theuerkauf, Anja, Montellano, Felipe A., Morbach, Caroline, Schmidt, Sein, Schreiber, Stefan, Steigerwald, Flo, Störk, Stefan, Maetzler, Walter, and Finke, Carsten

Published

2022

29. Comparing one dose of HPV vaccine in girls aged 9–14 years in Tanzania (DoRIS) with one dose of HPV vaccine in historical cohorts: an immunobridging analysis of a randomised controlled trial

Author

Baisley, Kathy, Kemp, Troy J, Kreimer, Aimée R, Basu, Partha, Changalucha, John, Hildesheim, Allan, Porras, Carolina, Whitworth, Hilary, Herrero, Rolando, Lacey, Charles J, Schiller, John T, Lucas, Eric, Mutani, Paul, Dillner, Joakim, Indangasi, Jackton, Muwonge, Richard, Hayes, Richard J, Pinto, Ligia A, and Watson-Jones, Deborah

Published

2022

30. Identifying Epstein–Barr virus peptide sequences associated with differential IgG antibody response

Author

Coghill, Anna E., Fang, Jianwen, Liu, Zhiwei, Chen, Chien-Jen, Jarrett, Ruth F., Hjalgrim, Henrik, Proietti, Carla, Yu, Kelly J., Hsu, Wan-Lun, Lou, Pei-Jen, Wang, Chen-Ping, Zhao, Yingdong, Doolan, Denise L., and Hildesheim, Allan

Published

2022

31. Perception of Children With Visible Untreated and Treated Caries (ECC-ET)

Author

Stiftung Universität Hildesheim and Claudia Tschammler, Postdoctoral Research Fellow

Published

2019

32. HPV16 infection decreases vaccine-induced HPV16 antibody avidity: the CVT trial

Author

Sabrina H. Tsang, John T. Schiller, Carolina Porras, Troy J. Kemp, Rolando Herrero, John Schussler, Monica S. Sierra, Bernal Cortes, Allan Hildesheim, Douglas R. Lowy, Ana Cecilia Rodríguez, Byron Romero, Nicolas Çuburu, Jaimie Z. Shing, Ligia A. Pinto, Joshua N. Sampson, Aimée R. Kreimer, and on behalf of the Costa Rica HPV Vaccine Trial Group

Subjects

Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract The HPV vaccine has shown sustained efficacy and consistent stabilization of antibody levels, even after a single dose. We defined the HPV16-VLP antibody avidity patterns over 11 years among women who received one- or three doses of the bivalent HPV vaccine in the Costa Rica HPV Vaccine Trial. Absolute HPV16 avidity was lower in women who received one compared to three doses, although the patterns were similar (increased in years 2 and 3 and remained stable over the remaining 8 years). HPV16 avidity among women who were HPV16-seropositive women at HPV vaccination, a marker of natural immune response to HPV16 infection, was significantly lower than those of HPV16-seronegative women, a difference that was more pronounced among one-dose recipients. No differences in HPV16 avidity were observed by HPV18 serostatus at vaccination, confirming the specificity of the findings. Importantly, point estimates for vaccine efficacy against incident, six-month persistent HPV16 infections was similar between women who were HPV16 seronegative and seropositive at the time of initial HPV vaccination for both one-dose and three-dose participants. It is therefore likely that this lower avidity level is still sufficient to enable antibody-mediated protection. It is encouraging for long-term HPV-vaccine protection that HPV16 antibody avidity was maintained for over a decade, even after a single dose.

Published

2022

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

Author

Safaeian, Mahboobeh, Sampson, Joshua, Pan, Yuanji, Porras, Carolina, Kemp, Troy, Herrero, Rolando, Quint, Wim, van Doorn, Leen, Schussler, John, Lowy, Douglas, Schiller, John, Schiffman, Mark, Rodriguez, Ana, Gail, Mitchell, Hildesheim, Allan, Gonzalez, Paula, Pinto, Ligia, and Kreimer, Aimée

Subjects

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

Abstract

BACKGROUND: 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. METHODS: 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. RESULTS: 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. CONCLUSIONS: 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

34. Characterization of the humoral immune response to the EBV proteome in extranodal NK/T-cell lymphoma

Author

Zhiwei Liu, Yomani D. Sarathkumara, John K. C. Chan, Yok-Lam Kwong, Tai Hing Lam, Dennis Kai Ming Ip, Brian C.-H. Chiu, Jun Xu, Yu-Chieh Su, Carla Proietti, Martha M. Cooper, Kelly J. Yu, Bryan Bassig, Raymond Liang, Wei Hu, Bu-Tian Ji, Anna E. Coghill, Ruth M. Pfeiffer, Allan Hildesheim, Nathaniel Rothman, Denise L. Doolan, and Qing Lan

Subjects

Medicine, Science

Abstract

Abstract Extranodal natural killer/T-cell lymphoma (NKTCL) is an aggressive malignancy that has been etiologically linked to Epstein-Barr virus (EBV) infection, with EBV gene transcripts identified in almost all cases. However, the humoral immune response to EBV in NKTCL patients has not been well characterized. We examined the antibody response to EBV in plasma samples from 51 NKTCL cases and 154 controls from Hong Kong and Taiwan who were part of the multi-center, hospital-based AsiaLymph case–control study. The EBV-directed serological response was characterized using a protein microarray that measured IgG and IgA antibodies against 202 protein sequences representing the entire EBV proteome. We analyzed 157 IgG antibodies and 127 IgA antibodies that fulfilled quality control requirements. Associations between EBV serology and NKTCL status were disproportionately observed for IgG rather than IgA antibodies. Nine anti-EBV IgG responses were significantly elevated in NKTCL cases compared with controls and had ORshighest vs. lowest tertile > 6.0 (Bonferroni-corrected P-values

Published

2021

35. Association between immunologic markers and cirrhosis in individuals with chronic hepatitis B

Author

Ilona Argirion, Ruth M. Pfeiffer, Tram Kim Lam, Thomas R. O’Brien, Kelly Yu, Katherine A. McGlynn, Jessica L. Petrick, Ligia Pinto, Chien-Jen Chen, Mei-Hsuan Lee, Allan Hildesheim, Hwai-I Yang, and Jill Koshiol

Subjects

Medicine, Science

Abstract

Abstract Host immune response and chronic inflammation associated with chronic hepatitis B virus (HBV) infection play a key role in the pathogenesis of liver diseases such as cirrhosis and hepatocellular carcinoma (HCC). We sampled 175 HCC, 117 cirrhotic and 165 non-cirrhotic controls from a prospective cohort study of chronically HBV-infected individuals. Multivariable polytomous logistic regression and canonical discriminant analysis (CDA) were used to compare baseline plasma levels for 102 markers in individuals who developed cirrhosis vs. controls and those who developed HCC vs. cirrhosis. Leave-one-out cross validation was used to generate receiver operating characteristic curves to compare the predictive ability of marker groups. After multivariable adjustment, HGF (Q4v1OR: 3.74; p-trend = 0.0001), SLAMF1 (Q4v1OR: 4.07; p-trend = 0.0001), CSF1 (Q4v1OR: 3.00; p-trend = 0.002), uPA (Q4v1OR: 3.36; p-trend = 0.002), IL-8 (Q4v1OR: 2.83; p-trend = 0.004), and OPG (Q4v1OR: 2.44; p-trend = 0.005) were all found to be associated with cirrhosis development compared to controls; these markers predicted cirrhosis with 69% accuracy. CDA analysis identified a nine marker model capable of predicting cirrhosis development with 79% accuracy. No markers were significantly different between HCC and cirrhotic participants. In this study, we assessed immunologic markers in relation to liver disease in chronically-HBV infected individuals. While validation in required, these findings highlight the importance of immunologic processes in HBV-related cirrhosis.

Published

2021

36. What contributes most to the SPPB and its subscores in hospitalized geriatric patients: an ICF model-based approach

Author

Kudelka, Jennifer, Geritz, Johanna, Welzel, Julius, Hildesheim, Hanna, Maetzler, Corina, Emmert, Kirsten, Niemann, Katharina, Hobert, Markus A., Pilotto, Andrea, Bergmann, Philipp, and Maetzler, Walter

Published

2022

37. Estimating vaccine effectiveness against SARS-CoV-2 infection, hospitalization and death from ecologic data in Costa Rica

Author

Fantin, Romain, Herrero, Rolando, Hildesheim, Allan, Barboza-Solís, Cristina, Aparicio, Amada, Prevots, D. Rebecca, Pfeiffer, Ruth M., and Gail, Mitchell H.

Published

2022

38. Oncogenic senescence: a multi-functional perspective

Author

Baker, Darren J, Alimirah, Fatouma, van Deursen, Jan M, Campisi, Judith, and Hildesheim, Jeffrey

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, Aging, Animals, Cell Transformation, Neoplastic, Cellular Senescence, Humans, Neoplasms, Tumor Microenvironment, cellular senescence, microenvironment, tumorigenesis, Oncology and carcinogenesis

Abstract

Cellular senescence is defined as an irreversible growth arrest with the acquisition of a distinctive secretome. The growth arrest is a potent anticancer mechanism whereas the secretome facilitates wound healing, tissue repair, and development. The senescence response has also become increasingly recognized as an important contributor to aging and age-related diseases, including cancer. Although oncogenic mutations are capable of inducing a beneficial senescence response that prevents the growth of premalignant cells and promotes cancer immune-surveillance, the secretome of senescent cells also includes factors with pro-tumorigenic properties. On June 23rd and 24th, 2016, the Division of Cancer Biology of the National Cancer Institute sponsored a workshop to discuss the complex role of cellular senescence in tumorigenesis with the goal to define the major challenges and opportunities within this important field of cancer research. Additionally, it was noted how the development of novel tools and technologies are required to accelerate research into a mechanistic understanding of senescent cells in carcinogenesis in order to overcome the current limitations in this exciting, yet ill-defined area.

Published

2017

39. U.S.-Japan cooperative medical sciences program: 22nd International Conference on Emerging Infectious Diseases in the Pacific Rim

Author

Lu, Kristina T., Yamamoto, Takuya, McDonald, David, Li, Wei, Tan, Marissa, Moi, Meng Ling, Park, Eun-Chung, Yoshimatsu, Kumiko, Ricciardone, Marie, Hildesheim, Allan, Totsuka, Yukari, Nanbo, Asuka, Putcharoen, Opass, Suwanpimolkul, Gompol, Jantarabenjakul, Watsamon, Paitoonpong, Leilani, Handley, F. Gray, Bernabe, K. Gayle, Noda, Masahiko, Sonoda, Miwa, Brennan, Patrick, Griffin, Diane E., and Kurane, Ichiro

Published

2021

40. Soluble cluster of differentiation 14 levels elevated in bile from gallbladder cancer cases from Shanghai, China

Author

Victoria L. Brun, Amanda F. Corbel, Ann W. Hsing, Troy J. Kemp, Alison L. Van Dyke, Allan Hildesheim, Bin Zhu, Yu-Tang Gao, Ligia A. Pinto, and Jill Koshiol

Subjects

Medicine, Science

Abstract

Abstract Elevated systemic levels of soluble cluster of differentiation 14 (sCD14) have been associated with gallbladder cancer (GBC), but the association with sCD14 levels within the gallbladder has not been investigated. Here, we evaluated sCD14 in the bile of 41 GBC cases and 117 gallstone controls with data on 65 bile inflammation markers. We examined the relationship between bile sCD14 levels and GBC using logistic regression and stratified the analysis by stage. We included GBC-associated inflammatory biomarkers in the model to evaluate the influence of local inflammation. Bile sCD14 levels (third versus first tertile) were associated with GBC (adjusted odds ratio [OR]: 3.0, 95% confidence interval [CI]: 1.2–8.0). The association was equally strong for stage I/II (OR: 3.3, 95% CI: 0.9–15.6) and stage III/IV (OR: 3.2, 95% CI: 1.0–12.4) cancers. Including the GBC-associated inflammatory markers in the model removed the association between bile sCD14 and GBC (OR: 1.0, 95% CI: 0.3–3.5). The findings suggest that immune activation within the gallbladder may be related to GBC development, and the effect of sCD14 is influenced by inflammation. Similar associations across tumor stages suggest that elevated bile sCD14 levels may reflect changes early in GBC pathogenesis. Associations between GBC and sCD14 levels in both bile and plasma suggest sCD14 could be a potential biomarker for GBC.

Published

2021

41. Predicting Language Function Post-Stroke: A Model-Based Structural Connectivity Approach

Author

Hildesheim, Franziska E., primary, Ophey, Anja, additional, Zumbansen, Anna, additional, Funck, Thomas, additional, Schuster, Tibor, additional, Jamison, Keith W., additional, Kuceyeski, Amy, additional, and Thiel, Alexander, additional

Published

2024

42. 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, Wacholder, Sholom, Schussler, John, Rodriguez, Ana, Porras, Carolina, Schiffman, Mark, Sidawy, Mary, Schiller, John, Lowy, Douglas, and Herrero, Rolando

Subjects

cervical cancer, clinical trial, human papillomaviruses, prevention, vaccines, 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

Abstract

BACKGROUND: Human 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. OBJECTIVES: To 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 DESIGN: We 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. RESULTS: Median 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. CONCLUSION: We 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

43. Inflammatory profiles in Chilean Mapuche and non-Mapuche women with gallstones at risk of developing gallbladder cancer

Author

Sarah S. Jackson, Vanessa Van De Wyngard, Ruth M. Pfeiffer, Paz Cook, Allan Hildesheim, Ligia A. Pinto, Sharon H. Jackson, Kelvin Choi, Ricardo A. Verdugo, Mara Cuevas, Cristian Yáñez, Eduardo Tobar-Calfucoy, Rocío Retamales-Ortega, Juan Carlos Araya, Catterina Ferreccio, and Jill Koshiol

Subjects

Medicine, Science

Abstract

Abstract Chile has high incidence rates of gallbladder cancer globally, particularly among Amerindian women, who also have a high prevalence of gallstones. We examined differences in inflammatory biomarkers between Mapuche and non-Mapuche women from the Chile Biliary Longitudinal Study, a cohort of women with ultrasound-detected gallstones. We randomly selected 200 Mapuche women frequency matched to non-Mapuche women on age and statin use Inflammatory biomarkers were analyzed using a multiplex assay and linear regression to assess associations of a priori markers (CCL20, CXCL10, IL-6, and IL-8) with ethnicity. Novel biomarkers were analyzed using exploratory factor analysis (EFA) and sufficient dimension reduction (SDR) to identify correlated marker groups, followed by linear regression to examine their association with ethnicity. The mean values of IL-8 were higher in Mapuche than non-Mapuche women (P = 0.04), while CCL20, CXCL10, and IL-6 did not differ significantly by ethnicity. EFA revealed two marker groups associated with ethnicity (P = 0.03 and P

Published

2021

44. Fitness costs of delayed pollination in a mixed-mating plant

Author

Hildesheim, Laura S., Opedal, Øystein H., Armbruster, W. Scott, and Pélabon, Christophe

Published

2019

45. FTY720 reactivates cryptococcal granulomas in mice through S1P receptor 3 on macrophages

Author

Bryan, Arielle M., You, Jeehyun Karen, McQuiston, Travis, Lazzarini, Cristina, Qiu, Zhijuan, Sheridan, Brian, Nuesslein-Hildesheim, Barbara, and Del Poeta, Maurizio

Subjects

Novartis Pharma AG, Analysis, Health aspects, Phosphates -- Analysis -- Health aspects, Macrophages -- Analysis -- Health aspects, Mycoses -- Health aspects -- Analysis, Sphingosine -- Analysis -- Health aspects, Medical research -- Analysis -- Health aspects, Infection -- Analysis -- Health aspects, Pharmaceutical industry -- Health aspects -- Analysis, Multiple sclerosis -- Analysis -- Health aspects, T cells -- Health aspects -- Analysis

Abstract

Introduction Cryptococcus spp. are important human fungal pathogens that cause life-threatening meningo-encephalitis in severely lymphopenic patients (1, 2). Cryptococcus neoformans causes approximately 223,100 cases of meningitis every year, resulting in [...], FTY720 is a treatment for relapsing remitting multiple sclerosis (MS). It is an analog of sphingosine-1-phosphate (S1P) and targets S1P receptors 1, 3, 4, and 5. Recent reports indicate an association between long-term exposure to FTY720 and cases of cryptococcal infection. Here, we studied the effect of FTY720 and its derivative, BAF312, which only target S1P receptors 1 and 5, in a mouse model of cryptococcal infection. We found that treatment with FTY720, but not with BAF312, led to decreased survival and increased organ burden in mouse cryptococcal granulomas. Both FTY720 and BAF312 caused a profound [CD4.sup.+] and [CD8.sup.+] T cell depletion in blood and lungs but only treatment with FTY720 led to cryptococcal reactivation. Treatment with FTY720, but not with BAF312, was associated with disorganization of macrophages and with M2 polarization at the granuloma site. In a cell system, FTY720 decreased phagocytosis and production of reactive oxygen species by macrophages, a phenotype recapitulated in the [S1pr3.sup.-/-] knockout macrophages. Our results suggest that FTY720 reactivates cryptococcosis from the granuloma through a S1P receptor 3-mediated mechanism and support the rationale for development of more-specific receptor modulators for therapeutic use of MS.

Published

2020

46. Therapy-Induced Senescence: Opportunities to Improve Anticancer Therapy

Author

Pataje G Prasanna, Deborah E Citrin, Jeffrey Hildesheim, Mansoor M Ahmed, Sundar Venkatachalam, Gabriela Riscuta, Dan Xi, Guangrong Zheng, Jan van Deursen, Jorg Goronzy, Stephen J Kron, Mitchell S Anscher, Norman E Sharpless, Judith Campisi, Stephen L Brown, Laura J Niedernhofer, Ana O’Loghlen, Alexandros G Georgakilas, Francois Paris, David Gius, David A Gewirtz, Clemens A Schmitt, Mohamed E Abazeed, James L Kirkland, Ann Richmond, Paul B Romesser, Scott W Lowe, Jesus Gil, Marc S Mendonca, Sandeep Burma, Daohong Zhou, and C Norman Coleman

Published

2021

47. 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, Hildesheim, Allan, Porras, Carolina, Herrero, Rolando, Wacholder, Sholom, Panagiotou, Orestis, Befano, Brian, Burk, Robert, and Schiffman, Mark

Subjects

HPV vaccine, HPV variants, cross-protection, Adolescent, Adult, Double-Blind Method, Female, Genetic Variation, Humans, Papillomaviridae, Papillomavirus Infections, Papillomavirus Vaccines, Young Adult

Abstract

BACKGROUND: Results 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. METHODS: A 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

48. The paradox of predictability provides a bridge between micro- and macroevolution

Author

Tsuboi, Masahito, Sztepanacz, Jacqueline, De Lisle, Stephen P., Voje, Kjetil L., Grabowski, Mark, Hopkins, Melanie J., Porto, Arthur, Balk, Meghan, Pontarp, Mikael, Rossoni, Daniela, Hildesheim, Laura S., Horta-Lacueva, Quentin J-B, Hohmann, Niklas, Holstad, Agnes, Lurig, Moritz, Milocco, Lisandro, Nilen, Sofie, Passarotto, Arianna, Svensson, Erik, I, Villegas, Cristina, Winslott, Erica, Liow, Lee Hsiang, Hunt, Gene, Love, Alan C., Houle, David, Tsuboi, Masahito, Sztepanacz, Jacqueline, De Lisle, Stephen P., Voje, Kjetil L., Grabowski, Mark, Hopkins, Melanie J., Porto, Arthur, Balk, Meghan, Pontarp, Mikael, Rossoni, Daniela, Hildesheim, Laura S., Horta-Lacueva, Quentin J-B, Hohmann, Niklas, Holstad, Agnes, Lurig, Moritz, Milocco, Lisandro, Nilen, Sofie, Passarotto, Arianna, Svensson, Erik, I, Villegas, Cristina, Winslott, Erica, Liow, Lee Hsiang, Hunt, Gene, Love, Alan C., and Houle, David

Abstract

The relationship between the evolutionary dynamics observed in contemporary populations (microevolution) and evolution on timescales of millions of years (macroevolution) has been a topic of considerable debate. Historically, this debate centers on inconsistencies between microevolutionary processes and macroevolutionary patterns. Here, we characterize a striking exception: emerging evidence indicates that standing variation in contemporary populations and macroevolutionary rates of phenotypic divergence is often positively correlated. This apparent consistency between micro- and macroevolution is paradoxical because it contradicts our previous understanding of phenotypic evolution and is so far unexplained. Here, we explore the prospects for bridging evolutionary timescales through an examination of this "paradox of predictability." We begin by explaining why the divergence-variance correlation is a paradox, followed by data analysis to show that the correlation is a general phenomenon across a broad range of temporal scales, from a few generations to tens of millions of years. Then we review complementary approaches from quantitative genetics, comparative morphology, evo-devo, and paleontology to argue that they can help to address the paradox from the shared vantage point of recent work on evolvability. In conclusion, we recommend a methodological orientation that combines different kinds of short-term and long-term data using multiple analytical frameworks in an interdisciplinary research program. Such a program will increase our general understanding of how evolution works within and across timescales.

Published

2024

49. Evaluation of walking activity and gait to identify physical and mental fatigue in neurodegenerative and immune disorders:preliminary insights from the IDEA-FAST feasibility study

Author

Hinchliffe, Chloe, Rehman, Rana Zia Ur, Pinaud, Clemence, Branco, Diogo, Jackson, Dan, Ahmaniemi, Teemu, Guerreiro, Tiago, Chatterjee, Meenakshi, Manyakov, Nikolay V., Pandis, Ioannis, Davies, Kristen, Macrae, Victoria, Aufenberg, Svenja, Paulides, Emma, Hildesheim, Hanna, Kudelka, Jennifer, Emmert, Kirsten, Van Gassen, Geert, Rochester, Lynn, van der Woude, C. Janneke, Reilmann, Ralf, Maetzler, Walter, Ng, Wan Fai, Del Din, Silvia, Hinchliffe, Chloe, Rehman, Rana Zia Ur, Pinaud, Clemence, Branco, Diogo, Jackson, Dan, Ahmaniemi, Teemu, Guerreiro, Tiago, Chatterjee, Meenakshi, Manyakov, Nikolay V., Pandis, Ioannis, Davies, Kristen, Macrae, Victoria, Aufenberg, Svenja, Paulides, Emma, Hildesheim, Hanna, Kudelka, Jennifer, Emmert, Kirsten, Van Gassen, Geert, Rochester, Lynn, van der Woude, C. Janneke, Reilmann, Ralf, Maetzler, Walter, Ng, Wan Fai, and Del Din, Silvia

Abstract

Background: Many individuals with neurodegenerative (NDD) and immune-mediated inflammatory disorders (IMID) experience debilitating fatigue. Currently, assessments of fatigue rely on patient reported outcomes (PROs), which are subjective and prone to recall biases. Wearable devices, however, provide objective and reliable estimates of gait, an essential component of health, and may present objective evidence of fatigue. This study explored the relationships between gait characteristics derived from an inertial measurement unit (IMU) and patient-reported fatigue in the IDEA-FAST feasibility study. Methods: Participants with IMIDs and NDDs (Parkinson's disease (PD), Huntington's disease (HD), rheumatoid arthritis (RA), systemic lupus erythematosus (SLE), primary Sjogren’s syndrome (PSS), and inflammatory bowel disease (IBD)) wore a lower-back IMU continuously for up to 10 days at home. Concurrently, participants completed PROs (physical fatigue (PF) and mental fatigue (MF)) up to four times a day. Macro (volume, variability, pattern, and acceleration vector magnitude) and micro (pace, rhythm, variability, asymmetry, and postural control) gait characteristics were extracted from the accelerometer data. The associations of these measures with the PROs were evaluated using a generalised linear mixed-effects model (GLMM) and binary classification with machine learning. Results: Data were recorded from 72 participants: PD = 13, HD = 9, RA = 12, SLE = 9, PSS = 14, IBD = 15. For the GLMM, the variability of the non-walking bouts length (in seconds) with PF returned the highest conditional R2, 0.165, and with MF the highest marginal R2, 0.0018. For the machine learning classifiers, the highest accuracy of the current analysis was returned by the micro gait characteristics with an intrasubject cross validation method and MF as 56.90% (precision = 43.9%, recall = 51.4%). Overall, the acceleration vector magnitude, bout length variation, postural control, and gait rhythm were

Published

2024

50. Effect of bivalent human papillomavirus vaccination on pregnancy outcomes: long term observational follow-up in the Costa Rica HPV Vaccine Trial.

Author

Panagiotou, Orestis A, Befano, Brian L, Gonzalez, Paula, Rodríguez, Ana Cecilia, Herrero, Rolando, Schiller, John T, Kreimer, Aimée R, Schiffman, Mark, Hildesheim, Allan, Wilcox, Allen J, Wacholder, Sholom, and Costa Rica HPV Vaccine Trial (CVT) Group (see end of manuscript for full list of investigators)

Subjects

Costa Rica HPV Vaccine Trial (CVT) Group, Humans, Abortion, Spontaneous, Pregnancy Outcome, Follow-Up Studies, Double-Blind Method, Maternal Age, Gestational Age, Pregnancy, Adolescent, Adult, Costa Rica, Female, Papillomavirus Vaccines, Young Adult, Clinical Trials and Supportive Activities, HPV and/or Cervical Cancer Vaccines, Vaccine Related, Clinical Research, Immunization, Infectious Diseases, Sexually Transmitted Infections, Cancer, Prevention, 3.4 Vaccines, Infection, Reproductive health and childbirth, General & Internal Medicine, Clinical Sciences, Public Health and Health Services

Abstract

OBJECTIVE:To examine the effect of the bivalent human papillomavirus (HPV) vaccine on miscarriage. DESIGN:Observational long term follow-up of a randomized, double blinded trial combined with an independent unvaccinated population based cohort. SETTING:Single center study in Costa Rica. PARTICIPANTS:7466 women in the trial and 2836 women in the unvaccinated cohort enrolled at the end of the randomized trial and in parallel with the observational trial component. INTERVENTION:Women in the trial were assigned to receive three doses of bivalent HPV vaccine (n=3727) or the control hepatitis A vaccine (n=3739). Crossover bivalent HPV vaccination occurred in the hepatitis A vaccine arm at the end of the trial. Women in the unvaccinated cohort received (n=2836) no vaccination. MAIN OUTCOME MEASURE:Risk of miscarriage, defined by the US Centers for Disease Control and Prevention as fetal loss within 20 weeks of gestation, in pregnancies exposed to bivalent HPV vaccination in less than 90 days and any time from vaccination compared with pregnancies exposed to hepatitis A vaccine and pregnancies in the unvaccinated cohort. RESULTS:Of 3394 pregnancies conceived at any time since bivalent HPV vaccination, 381 pregnancies were conceived less than 90 days from vaccination. Unexposed pregnancies comprised 2507 pregnancies conceived after hepatitis A vaccination and 720 conceived in the unvaccinated cohort. Miscarriages occurred in 451 (13.3%) of all exposed pregnancies, in 50 (13.1%) of the pregnancies conceived less than 90 days from bivalent HPV vaccination, and in 414 (12.8%) of the unexposed pregnancies, of which 316 (12.6%) were in the hepatitis A vaccine group and 98 (13.6%) in the unvaccinated cohort. The relative risk of miscarriage for pregnancies conceived less than 90 days from vaccination compared with all unexposed pregnancies was 1.02 (95% confidence interval 0.78 to 1.34, one sided P=0.436) in unadjusted analyses. Results were similar after adjusting for age at vaccination (relative risk 1.15, one sided P=0.17), age at conception (1.03, P=0.422), and calendar year (1.06, P=0.358), and in stratified analyses. Among pregnancies conceived at any time from bivalent HPV vaccination, exposure was not associated with an increased risk of miscarriage overall or in subgroups, except for miscarriages at weeks 13-20 of gestation (relative risk 1.35, 95% confidence interval 1.02 to 1.77, one sided P=0.017). CONCLUSIONS:There is no evidence that bivalent HPV vaccination affects the risk of miscarriage for pregnancies conceived less than 90 days from vaccination. The increased risk estimate for miscarriages in a subgroup of pregnancies conceived any time after vaccination may be an artifact of a thorough set of sensitivity analyses, but since a genuine association cannot totally be ruled out, this signal should nevertheless be explored further in existing and future studies.Trial registration Clinicaltrials.gov NCT00128661 and NCT01086709.

Published

2015