Your search keyword '"Gellert, Lan"' showing total 21 results

1. Pathological characterization and clinical outcome of penile intraepithelial neoplasia variants: a North American series

Author

Straub Hogan, Melissa M., Spieker, Andrew J., Orejudos, Michael, Gheit, Tarik, Herfs, Michael, Tommasino, Massimo, Sanchez, Diego F., Fernandez-Nestosa, Maria Jose, Pena, Maria Del Carmen Rodriguez, Gordetsky, Jennifer B., Epstein, Jonathan I., Canete-Portillo, Sofia, Gellert, Lan L., Prieto Granada, Carlos Nicolas, Magi-Galluzzi, Cristina, Cubilla, Antonio L., and Giannico, Giovanna A.

Abstract

Penile intraepithelial neoplasia (PeIN) is classified as human papillomavirus (HPV)- and non-HPV-related. This classification is associated with distinct morphologic subtypes. The natural history and prognosis of PeIN subtypes are not well known. This study aims to evaluate clinicopathological features, HPV status, and outcome of PeIN subtypes. Eighty-two lesions from 64 patients with isolated PeIN were retrospectively reviewed. Mean age was 59 years. Lesions were multicentric in 34% of patients and affected glans (33%), shaft (26%), and foreskin (20%). Histologically, 22% of patients had coexisting lesions, classified as hybrid and mixed. HPV-related PeIN (97%) included basaloid (59%), warty (8%), warty-basaloid (8%), hybrid (19%) and mixed (3%) types. P16 and HPV positivity occurred in 99% and 82% of lesions, respectively. HPV 16 was more common in basaloid PeIN. Multiple genotypes were detected in 35%, more commonly in hybrid PeIN (P= 0.051). Positive margins occurred in 63% of excisions. PeIN recurred in 48% of excisions and 30% of overall repeated procedures, and progression to invasive carcinoma occurred in 2%. At follow-up, 86% of patients had no evidence of disease and 12% were alive with disease. Lichen sclerosus occurred in non-HPV and HPV-related PeIN (100% and 47%).

Published

2022

2. Pathological characterization and clinical outcome of penile intraepithelial neoplasia variants: a North American series

Author

Straub Hogan, Melissa M., Spieker, Andrew J., Orejudos, Michael, Gheit, Tarik, Herfs, Michael, Tommasino, Massimo, Sanchez, Diego F., Fernandez-Nestosa, Maria Jose, Pena, Maria Del Carmen Rodriguez, Gordetsky, Jennifer B., Epstein, Jonathan I., Canete-Portillo, Sofia, Gellert, Lan L., Prieto Granada, Carlos Nicolas, Magi-Galluzzi, Cristina, Cubilla, Antonio L., and Giannico, Giovanna A.

Abstract

Penile intraepithelial neoplasia (PeIN) is classified as human papillomavirus (HPV)- and non-HPV-related. This classification is associated with distinct morphologic subtypes. The natural history and prognosis of PeIN subtypes are not well known. This study aims to evaluate clinicopathological features, HPV status, and outcome of PeIN subtypes. Eighty-two lesions from 64 patients with isolated PeIN were retrospectively reviewed. Mean age was 59 years. Lesions were multicentric in 34% of patients and affected glans (33%), shaft (26%), and foreskin (20%). Histologically, 22% of patients had coexisting lesions, classified as hybrid and mixed. HPV-related PeIN (97%) included basaloid (59%), warty (8%), warty-basaloid (8%), hybrid (19%) and mixed (3%) types. P16 and HPV positivity occurred in 99% and 82% of lesions, respectively. HPV 16 was more common in basaloid PeIN. Multiple genotypes were detected in 35%, more commonly in hybrid PeIN (P= 0.051). Positive margins occurred in 63% of excisions. PeIN recurred in 48% of excisions and 30% of overall repeated procedures, and progression to invasive carcinoma occurred in 2%. At follow-up, 86% of patients had no evidence of disease and 12% were alive with disease. Lichen sclerosus occurred in non-HPV and HPV-related PeIN (100% and 47%).

Published

2022

3. Targeted Mutational Analysis of Cortisol-Producing Adenomas

Author

Rege, Juilee, Hoxie, Jessie, Liu, Chia-Jen, Cash, Morgan N, Luther, James M, Gellert, Lan, Turcu, Adina F, Else, Tobias, Giordano, Thomas J, Udager, Aaron M, Rainey, William E, and Nanba, Kazutaka

Published

2022

4. Genetic Characteristics of Aldosterone-Producing Adenomas in Blacks.

Author

Nanba, Kazutaka, Omata, Kei, Gomez-Sanchez, Celso E., Stratakis, Constantine A., Demidowich, Andrew P., Suzuki, Mari, Thompson, Lester D. R., Cohen, Debbie L., Luther, James M., Gellert, Lan, Vaidya, Anand, Barletta, Justine A., Else, Tobias, Giordano, Thomas J., Tomlins, Scott A., and Rainey, William E.

Abstract

Somatic mutations have been identified in aldosterone-producing adenomas (APAs) in genes that include KCNJ5, ATP1A1, ATP2B3, and CACNA1D. Based on independent studies, there appears to be racial differences in the prevalence of somatic KCNJ5 mutations, particularly between East Asians and Europeans. Despite the high cardiovascular disease mortality of blacks, there have been no studies focusing on somatic mutations in APAs in this population. In the present study, we investigated genetic characteristics of APAs in blacks using a CYP11B2 (aldosterone synthase) immunohistochemistry-guided next-generation sequencing approach. The adrenal glands with adrenocortical adenomas from 79 black patients with primary aldosteronism were studied. Seventy-three tumors from 69 adrenal glands were confirmed to be APAs by CYP11B2 immunohistochemistry. Sixty-five of 73 APAs (89%) had somatic mutations in aldosterone-driver genes. Somatic CACNA1D mutations were the most prevalent genetic alteration (42%), followed by KCNJ5 (34%), ATP1A1 (8%), and ATP2B3 mutations (4%). CACNA1D mutations were more often observed in APAs from males than those from females (55% versus 29%, P=0.033), whereas KCNJ5 mutations were more prevalent in APAs from females compared with those from males (57% versus 13%, P<0.001). No somatic mutations in aldosterone-driver genes were identified in tumors without CYP11B2 expression. In conclusion, 89% of APAs in blacks harbor aldosterone-driving mutations, and unlike Europeans and East Asians, the most frequently mutated aldosterone-driver gene was CACNA1D. Determination of racial differences in the prevalence of aldosterone-driver gene mutations may facilitate the development of personalized medicines for patients with primary aldosteronism. [ABSTRACT FROM AUTHOR]

Published

2019

5. Core Needle Biopsy and Fine Needle Aspiration Alone or in Combination: Diagnostic Accuracy and Impact on Management of Renal Masses.

Author

Cate, Frances, Kapp, Meghan E., Arnold, Shanna A., Gellert, Lan L., Hameed, Omar, Clark, Peter E., Wile, Geoffrey, Coogan, Alice, and Giannico, Giovanna A.

Subjects

CORE needle biopsy, KIDNEY tumors, RETROSPECTIVE studies, PUBLIC health, DIAGNOSIS, TUMOR treatment

Abstract

Purpose Fine needle aspiration with and without concurrent core needle biopsy is a minimally invasive method to diagnose and assist in management of renal masses. We assessed the pathological accuracy of fine needle aspiration compared to and associated with core needle biopsy and the impact on management. Materials and Methods We performed a single institution, retrospective study of 342 cases from 2001 to 2015 with small and large renal masses (4 or less and greater than 4 cm, respectively). Diagnostic and concordance rates, and the impact on management were analyzed. Results Adequacy rates for fine needle aspiration only, core needle biopsy only and fine needle aspiration plus core needle biopsy were 21%, 12% and 8% (aspiration vs aspiration plus biopsy p <0.026). In the aspiration plus biopsy group adding aspiration to biopsy and biopsy to aspiration reduced the inadequacy rate from 23% to 8% and from 27% to 8% for a total reduction rate of 15% and 19%, respectively, corresponding to 32 cases (9.3%). Rapid on-site examination contributed to a 22.5% improvement in fine needle aspiration adequacy rates. In this cohort 30% of aspiration only, 5% of biopsy only and 12% of aspiration plus biopsy could not be subtyped (aspiration vs biopsy p <0.0001, aspiration vs aspiration plus biopsy p <0.0127 and biopsy vs aspiration plus biopsy p = 0.06). The diagnostic concordance rate with surgical resection was 99%. Conversion of an inadequate specimen to an adequate one by a concurrent procedure impacted treatment in at least 29 of 32 patients. Limitations include the retrospective design and accuracy measurement based on surgical intervention. Conclusions Fine needle aspiration plus core needle biopsy vs at least fine needle aspiration alone may improve diagnostic yield when sampling renal masses but it has subtyping potential similar to that of core needle biopsy only. [ABSTRACT FROM AUTHOR]

Published

2017

6. Primary Carcinoid Tumor of the Renal Pelvis Arising From Intestinal Metaplasia: An Unusual Histogenetic Pathway?

Author

Kuba, Maria G., Wasserman, Allison, Vnencak-Jones, Cindy L., Bridge, Julia A., Gellert, Lan, Hameed, Omar, and Giannico, Giovanna A.

Published

2017

7. New and Emerging Diagnostic and Prognostic Immunohistochemical Biomarkers in Prostate Pathology

Author

Giannico, Giovanna A., Arnold, Shanna A., Gellert, Lan L., and Hameed, Omar

Abstract

The diagnosis of minimal prostatic adenocarcinoma can be challenging on prostate needle biopsy, and immunohistochemistry may be used to support the diagnosis of cancer. The International Society of Urologic Pathology currently recommends the use of the basal cell markers high–molecular-weight cytokeraratin and p63, and α-methylacyl-coenzyme-A racemase. However, there are caveats associated with the interpretation of these markers, particularly with benign mimickers. Another issue is that of early detection of presence and progression of disease and prediction of recurrence after clinical intervention. There remains a lack of reliable biomarkers to accurately predict low-risk cancer and avoid over treatment. As such, aggressive forms of prostate cancer may be missed and indolent disease may be subjected to unnecessary radical therapy. New biomarker discovery promises to improve early detection and prognosis and to provide targets for therapeutic interventions. In this review, we present the emerging immunohistochemical biomarkers of prostate cancer PTEN, ERG, FASN, MAGI-2, and SPINK1, and address their diagnostic and prognostic advantages and limitations.

Published

2017

8. Lack of P16ink4a Over Expression in Penile Squamous Cell Carcinoma is Associated with Recurrence after Lymph Node Dissection.

Author

Tang, Dominic H., Clark, Peter E., Giannico, Giovanna, Hameed, Omar, Chang, Sam S., and Gellert, Lan L.

Subjects

PENILE cancer, SQUAMOUS cell carcinoma, PAPILLOMAVIRUS diseases, GENETIC overexpression, DISEASE relapse, LYMPH node surgery, DISEASE risk factors

Abstract

Purpose There have been conflicting data in studies on the prognostic role of high risk human papillomavirus in penile squamous cell carcinoma. Using P16 ink4a over expression as a surrogate marker for high risk human papillomavirus, we evaluated high risk human papillomavirus status with respect to various clinical features, including recurrence and overall survival, among others. Materials and Methods P16 ink4a over expression was evaluated by immunohistochemistry for 119 consecutive patients with penile squamous cell carcinoma. Several variables were recorded including age, stage, histological grade, lymph node status, lymphovascular invasion, metastasis and recurrence. Median followup was 30 months. Results P16 ink4a over expression was detected in 49.5% (59 of 119) of samples. There was no significant difference between P16 ink4a negative and P16 ink4a positive tumors in terms of stage (p = 0.518), histological grade (p = 0.225), lymphovascular invasion (p = 0.388), overall survival (p = 0.156) or lymph node metastasis (p = 0.748). P16 ink4a negative tumors were more likely to recur overall (p = 0.04), especially if patients had positive lymph nodes at diagnosis (p = 0.002). Conclusions These data suggest that P16 ink4a /high risk human papillomavirus status is associated with recurrence, especially in patients with positive lymph nodes at diagnosis. Thus, patients with P16 ink4a negative penile cancer, particularly those with lymph node metastases, may warrant closer observation after surgery. [ABSTRACT FROM AUTHOR]

Published

2015

9. Loss of FOXA1 Drives Sexually Dimorphic Changes in Urothelial Differentiation and Is an Independent Predictor of Poor Prognosis in Bladder Cancer

Author

Reddy, Opal L., Cates, Justin M., Gellert, Lan L., Crist, Henry S., Yang, Zhaohai, Yamashita, Hironobu, Taylor, John A., Smith, Joseph A., Chang, Sam S., Cookson, Michael S., You, Chaochen, Barocas, Daniel A., Grabowska, Magdalena M., Ye, Fei, Wu, Xue-Ru, Yi, Yajun, Matusik, Robert J., Kaestner, Klaus H., Clark, Peter E., and DeGraff, David J.

Abstract

We previously found loss of forkhead box A1 (FOXA1) expression to be associated with aggressive urothelial carcinoma of the bladder, as well as increased tumor proliferation and invasion. These initial findings were substantiated by The Cancer Genome Atlas, which identified FOXA1mutations in a subset of bladder cancers. However, the prognostic significance of FOXA1 inactivation and the effect of FOXA1 loss on urothelial differentiation remain unknown. Application of a univariate analysis (log-rank) and a multivariate Cox proportional hazards regression model revealed that loss of FOXA1 expression is an independent predictor of decreased overall survival. An ubiquitin Cre-driven system ablating Foxa1expression in urothelium of adult mice resulted in sex-specific histologic alterations, with male mice developing urothelial hyperplasia and female mice developing keratinizing squamous metaplasia. Microarray analysis confirmed these findings and revealed a significant increase in cytokeratin 14 expression in the urothelium of the female Foxa1knockout mouse and an increase in the expression of a number of genes normally associated with keratinocyte differentiation. IHC confirmed increased cytokeratin 14 expression in female bladders and additionally revealed enrichment of cytokeratin 14–positive basal cells in the hyperplastic urothelial mucosa in male Foxa1knockout mice. Analysis of human tumor specimens confirmed a significant relationship between loss of FOXA1 and increased cytokeratin 14 expression.

Published

2015

10. Plasma Epstein-Barr virus DNA predicts outcome in advanced Hodgkin lymphoma: correlative analysis from a large North American cooperative group trial

Author

Kanakry, Jennifer A., Li, Hailun, Gellert, Lan L., Lemas, M. Victor, Hsieh, Wen-son, Hong, Fangxin, Tan, King L., Gascoyne, Randy D., Gordon, Leo I., Fisher, Richard I., Bartlett, Nancy L., Stiff, Patrick, Cheson, Bruce D., Advani, Ranjana, Miller, Thomas P., Kahl, Brad S., Horning, Sandra J., and Ambinder, Richard F.

Abstract

Epstein-Barr virus (EBV) is associated with Hodgkin lymphoma (HL) and can be detected by in situ hybridization (ISH) of viral nucleic acid (EBER) in tumor cells. We sought to determine whether plasma EBV-DNA could serve as a surrogate for EBER-ISH and to explore its prognostic utility in HL. Specimens from the Cancer Cooperative Intergroup Trial E2496 were used to compare pretreatment plasma EBV-DNA quantification with EBV tumor status by EBER-ISH. A cutoff of >60 viral copies/100 µL plasma yielded 96% concordance with EBER-ISH. Pretreatment and month 6 plasma specimens were designated EBV(-) or EBV(+) by this cutoff. Patients with pretreatment EBV(+) plasma (n = 54) had inferior failure-free survival (FFS) compared with those with pretreatment EBV(-) plasma (n = 274), log-rank P= .009. By contrast, no difference in FFS was observed when patients were stratified by EBER-ISH. Pretreatment plasma EBV positivity was an independent predictor of treatment failure on multivariate analyses. At month 6, plasma EBV(+) patients (n = 7) had inferior FFS compared with plasma EBV(-) patients (n = 125), log-rank P= .007. These results confirm that plasma EBV-DNA is highly concordant with EBER-ISH in HL and suggest that it may have prognostic utility both at baseline and after therapy. This trial was registered at www.clinicaltrials.govas #NCT00003389.

Published

2013

11. Plasma Epstein-Barr virus DNA predicts outcome in advanced Hodgkin lymphoma: correlative analysis from a large North American cooperative group trial

Author

Kanakry, Jennifer A., Li, Hailun, Gellert, Lan L., Lemas, M. Victor, Hsieh, Wen-son, Hong, Fangxin, Tan, King L., Gascoyne, Randy D., Gordon, Leo I., Fisher, Richard I., Bartlett, Nancy L., Stiff, Patrick, Cheson, Bruce D., Advani, Ranjana, Miller, Thomas P., Kahl, Brad S., Horning, Sandra J., and Ambinder, Richard F.

Abstract

Epstein-Barr virus (EBV) is associated with Hodgkin lymphoma (HL) and can be detected by in situ hybridization (ISH) of viral nucleic acid (EBER) in tumor cells. We sought to determine whether plasma EBV-DNA could serve as a surrogate for EBER-ISH and to explore its prognostic utility in HL. Specimens from the Cancer Cooperative Intergroup Trial E2496 were used to compare pretreatment plasma EBV-DNA quantification with EBV tumor status by EBER-ISH. A cutoff of >60 viral copies/100 µL plasma yielded 96% concordance with EBER-ISH. Pretreatment and month 6 plasma specimens were designated EBV(-) or EBV(+) by this cutoff. Patients with pretreatment EBV(+) plasma (n = 54) had inferior failure-free survival (FFS) compared with those with pretreatment EBV(-) plasma (n = 274), log-rank P = .009. By contrast, no difference in FFS was observed when patients were stratified by EBER-ISH. Pretreatment plasma EBV positivity was an independent predictor of treatment failure on multivariate analyses. At month 6, plasma EBV(+) patients (n = 7) had inferior FFS compared with plasma EBV(-) patients (n = 125), log-rank P = .007. These results confirm that plasma EBV-DNA is highly concordant with EBER-ISH in HL and suggest that it may have prognostic utility both at baseline and after therapy. This trial was registered at www.clinicaltrials.gov as #NCT00003389.

Published

2013

12. HMGA2: A biomarker significantly overexpressed in high-grade ovarian serous carcinoma

Author

Mahajan, Aparna, Liu, Zhaojian, Gellert, Lan, Zou, Xuanyi, Yang, Guangyu, Lee, Peng, Yang, Ximing, and Wei, Jian-Jun

Abstract

Ovarian carcinoma consists of a group of histologically heterogeneous diseases involving distinct tumorigenic pathways. High-grade papillary serous carcinoma of the ovary is commonly associated with p53mutations. HMGA2, an oncofetal protein, is found to be overexpressed in ovarian cancer. To study the function of HMGA2in ovarian cancer, it is important to know which subtypes of ovarian cancer are associated with HMGA2overexpression. In this study, we collected six different types of ovarian cancer and examined HMGA2expression by immunohistochemistry, along with HMGA1, p53and Ki-67. We found that HMGA2overexpression was significantly higher in high-grade papillary serous carcinoma (64%) and carcinosarcoma (60%) than in other types of ovarian cancers (7–23%). HMGA2overexpression was moderately associated with dominant p53mutations (R=0.51). In addition, the microRNA in situanalysis revealed that let-7b, the HMGA2-negative regulators, were significantly lost in high-grade serous carcinoma. Our findings suggest that HMGA2is an important molecular change significantly related to high-grade papillary serous carcinoma and is less common in other histological types of ovarian cancer.

Published

2010

13. HMGA2: A biomarker significantly overexpressed in high-grade ovarian serous carcinoma

Author

Mahajan, Aparna, Liu, Zhaojian, Gellert, Lan, Zou, Xuanyi, Yang, Guangyu, Lee, Peng, Yang, Ximing, and Wei, Jian-Jun

Abstract

Ovarian carcinoma consists of a group of histologically heterogeneous diseases involving distinct tumorigenic pathways. High-grade papillary serous carcinoma of the ovary is commonly associated with p53 mutations. HMGA2, an oncofetal protein, is found to be overexpressed in ovarian cancer. To study the function of HMGA2 in ovarian cancer, it is important to know which subtypes of ovarian cancer are associated with HMGA2 overexpression. In this study, we collected six different types of ovarian cancer and examined HMGA2 expression by immunohistochemistry, along with HMGA1, p53 and Ki-67. We found that HMGA2 overexpression was significantly higher in high-grade papillary serous carcinoma (64%) and carcinosarcoma (60%) than in other types of ovarian cancers (7–23%). HMGA2 overexpression was moderately associated with dominant p53 mutations (R=0.51). In addition, the microRNA in situ analysis revealed that let-7b, the HMGA2-negative regulators, were significantly lost in high-grade serous carcinoma. Our findings suggest that HMGA2 is an important molecular change significantly related to high-grade papillary serous carcinoma and is less common in other histological types of ovarian cancer.

Published

2010

14. Circulating clonotypic B cells in classic Hodgkin lymphoma

Author

Jones, Richard J., Gocke, Christopher D., Kasamon, Yvette L., Miller, Carole B., Perkins, Brandy, Barber, James P., Vala, Milada S., Gerber, Jonathan M., Gellert, Lan L., Siedner, Mark, Lemas, M. Victor, Brennan, Sarah, Ambinder, Richard F., and Matsui, William

Abstract

Although Hodgkin and Reed-Sternberg (HRS) cells are B lymphoid cells, they are unlike any normal cells of that lineage. Moreover, the limited proliferative potential of HRS cells belies the clinical aggressiveness of Hodgkin lymphoma (HL). More than 20 years ago, the L428 HL cell line was reported to contain a small population of phenotypic B cells that appeared responsible for the continued generation of HRS cells. This observation, however, has never been corroborated, and such clonotypic B cells have never been documented in HL patients. We found that both the L428 and KM-H2 HL cell lines contained rare B-cell subpopulations responsible for the generation and maintenance of the predominant HRS cell population. The B cells within the HL cell lines expressed immunoglobulin light chain, the memory B-cell antigen CD27, and the stem cell marker aldehyde dehydrogenase (ALDH). Clonal CD27+ALDHhighB cells, sharing immunoglobulin gene rearrangements with lymph node HRS cells, were also detected in the blood of most newly diagnosed HL patients regardless of stage. Although the clinical significance of circulating clonotypic B cells in HL remains unclear, these data suggest they may be the initiating cells for HL.

Published

2009

15. Circulating clonotypic B cells in classic Hodgkin lymphoma

Author

Jones, Richard J., Gocke, Christopher D., Kasamon, Yvette L., Miller, Carole B., Perkins, Brandy, Barber, James P., Vala, Milada S., Gerber, Jonathan M., Gellert, Lan L., Siedner, Mark, Lemas, M. Victor, Brennan, Sarah, Ambinder, Richard F., and Matsui, William

Abstract

Although Hodgkin and Reed-Sternberg (HRS) cells are B lymphoid cells, they are unlike any normal cells of that lineage. Moreover, the limited proliferative potential of HRS cells belies the clinical aggressiveness of Hodgkin lymphoma (HL). More than 20 years ago, the L428 HL cell line was reported to contain a small population of phenotypic B cells that appeared responsible for the continued generation of HRS cells. This observation, however, has never been corroborated, and such clonotypic B cells have never been documented in HL patients. We found that both the L428 and KM-H2 HL cell lines contained rare B-cell subpopulations responsible for the generation and maintenance of the predominant HRS cell population. The B cells within the HL cell lines expressed immunoglobulin light chain, the memory B-cell antigen CD27, and the stem cell marker aldehyde dehydrogenase (ALDH). Clonal CD27+ALDHhigh B cells, sharing immunoglobulin gene rearrangements with lymph node HRS cells, were also detected in the blood of most newly diagnosed HL patients regardless of stage. Although the clinical significance of circulating clonotypic B cells in HL remains unclear, these data suggest they may be the initiating cells for HL.

Published

2009

16. Clonal immunoglobulin DNA in the plasma of patients with AIDS lymphoma

Author

Wagner-Johnston, Nina D., Gellert, Lan, Gocke, Christopher D., Lemas, Victor M., Lee, Jeannette, Martínez-Maza, Otoniel, and Ambinder, Richard F.

Abstract

Immunoglobulin (Ig) gene rearrangements are used to define clonality of suspected B-lineage malignancy in tissue samples. To determine whether such rearrangements could be identified in plasma, we screened plasma from 14 consecutive patients with AIDS-related lymphoma with multiplex Ig primers. Clonally rearranged Ig DNA was detected in plasma from 7 of 14 patients. Patients in whom clonal Ig DNA remained detectable after combination chemotherapy died with lymphoma. Tumor was available from 1 patient, and the IgH amplification products from plasma and tumor were sequenced and confirmed to be identical. Ig DNA rearrangements in plasma may be useful as a lymphoma-specific tumor marker, and failure to clear clonal Ig DNA may identify patients at high risk for failure of standard therapy.

Published

2011

17. Clonal immunoglobulin DNA in the plasma of patients with AIDS lymphoma

Author

Wagner-Johnston, Nina D., Gellert, Lan, Gocke, Christopher D., Lemas, Victor M., Lee, Jeannette, Martínez-Maza, Otoniel, and Ambinder, Richard F.

Abstract

Immunoglobulin (Ig) gene rearrangements are used to define clonality of suspected B-lineage malignancy in tissue samples. To determine whether such rearrangements could be identified in plasma, we screened plasma from 14 consecutive patients with AIDS-related lymphoma with multiplex Ig primers. Clonally rearranged Ig DNA was detected in plasma from 7 of 14 patients. Patients in whom clonal Ig DNA remained detectable after combination chemotherapy died with lymphoma. Tumor was available from 1 patient, and the IgH amplification products from plasma and tumor were sequenced and confirmed to be identical. Ig DNA rearrangements in plasma may be useful as a lymphoma-specific tumor marker, and failure to clear clonal Ig DNA may identify patients at high risk for failure of standard therapy.

Published

2011

18. MP49-01 FOXA1 LOSS IS ASSOCIATED WITH POOR PROGNOSIS AND SEX-DEPENDENT PHENOTYPES FOLLOWING GENETIC INACTIVATION.

Author

Lin-Tsai Reddy, Opal, Cates, Justin, Gellert, Lan, Yamashita, Hironobu, Taylor, John, Smith Jr., Joseph, Chang, Sam, Cookson, Michael, Barocas, Daniel, Grabowska, Magdalena, Ye, Fei, Wu, Xue-Ru, Yi, Yajun, Matusik, Robert, Kaestner, Klaus, Clark, Peter, and DeGraff, David

Subjects

DNA-binding proteins, PHENOTYPES, GENETIC disorders, MEDICAL research, UROLOGY, PROGNOSIS

Published

2015

19. Serum Biomarkers Predict Outcomes in Advanced Hodgkin Lymphoma Independent of International Prognostic Score (IPS) and Treatment: Correlative Analysis from a Large North American Cooperative Group Trial

Author

Kanakry, Jennifer A., Hong, Fangxin, Martinez-Maza, Otoniel, Horning, Sandra J, Gordon, Leo I., Gascoyne, Randy D, Gellert, Lan L, Lemas, M. Victor, Cheson, Bruce, Advani, Ranjana H, Pohlman, Brad, Kenkre, Vaishalee P., Winter, Jane N., Stiff, Patrick J., Tuscano, Joseph, Friedberg, Jonathan, Dreosti, Lydia, Fisher, Richard I., Laneuville, Pierre, Kahl, Brad S, and Ambinder, Richard F.

Abstract

Cheson: Pharmacyclics: Membership on an entity's Board of Directors or advisory committees, Research Funding; Gilead: Research Funding; Acerta: Membership on an entity's Board of Directors or advisory committees, Research Funding. Winter:Pharmacyclics: Research Funding; Medivation: Other: Provision of investigational agent for clinical trial; GSK: Research Funding; Seattle Genetics: Research Funding. Friedberg:Bayer: Honoraria, Other: Data Safety Monitoring Board. Kahl:This study was coordinated by the ECOG-ACRIN Cancer Research Group (Robert L. Comis, MD and Mitchell D. Schnall, MD, PhD, Group Co-Chairs) and supported by the National Cancer Institute of the National Institutes of Health under the following award number: Research Funding.

Published

2016

20. Serum Biomarkers Predict Outcomes in Advanced Hodgkin Lymphoma Independent of International Prognostic Score (IPS) and Treatment: Correlative Analysis from a Large North American Cooperative Group Trial

Author

Kanakry, Jennifer A., Hong, Fangxin, Martinez-Maza, Otoniel, Horning, Sandra J, Gordon, Leo I., Gascoyne, Randy D, Gellert, Lan L, Lemas, M. Victor, Cheson, Bruce, Advani, Ranjana H, Pohlman, Brad, Kenkre, Vaishalee P., Winter, Jane N., Stiff, Patrick J., Tuscano, Joseph, Friedberg, Jonathan, Dreosti, Lydia, Fisher, Richard I., Laneuville, Pierre, Kahl, Brad S, and Ambinder, Richard F.

Abstract

Introduction: Progress in the treatment of patients with classical Hodgkin lymphoma (cHL) depends on identifying methods to better risk-stratify patients and assess prognosis and treatment response. While prognostic scores based on clinical characteristics have utility, inflammatory markers and signaling proteins may better reflect tumor biology, the microenvironment, or host response and might serve as prognostic factors. Increased expression of tumor-associated macrophage markers in tumor tissue, such as CD68 or CD163, has been shown to be associated with inferior survival outcomes in cHL patients. Blood-based markers are more practical in that specimens are readily and serially obtainable. Such markers, if shown to track with tumor response and/or prognosticate outcomes, can be used throughout treatment and follow-up. Some soluble markers, such as TARC (chemokine (C-C motif) ligand (CCL)-17) and soluble CD163 (sCD163), have been shown to reflect tumor burden and active disease, and markers such as soluble CD30 (sCD30), interleukin (IL)-6, chemokine (C-X-C motif) ligand (CXCL)-10/IP10, and IL-2 receptor have been associated with failure-free survival (FFS).

Published

2016

21. MP49-04 ROLE OF NUCLEAR AND CYTOPLASMIC TBLR1 IN PROSTATE CANCER.

Author

Daniels, Garrett, Li, Yirong, Gellert, Lan Lin, Melamed, Jonathan, Wu, Xinyu, Zhang, David, Meruelo, Daniel, Logan, Susan, Basch, Ross, and Lee, Peng

Published

2014