Your search keyword '"Dhananjay A. Chitale"' showing total 5 results

1. Race Differences in Telomere Length in Benign Prostate Biopsies and Subsequent Risk of Prostate Cancer

Author

Benjamin A. Rybicki, Sudha M. Sadasivan, Yalei Chen, Ian Loveless, Nilesh S. Gupta, Dhananjay A. Chitale, Sean R. Williamson, Andrew G. Rundle, and Deliang L. Tang

Subjects

Male, Oncology, Epidemiology, Risk Factors, Biopsy, Case-Control Studies, Leukocytes, Prostate, Humans, Prostatic Neoplasms, Telomere, Article, Race Factors

Abstract

Background: Telomere shortening is linked to aging and may be associated with increased risk for cancer. Most cancer studies have used telomere length in leukocytes rather than in the target tissue of cancer origin. Methods: A case–control study of 524 case–control pairs with a benign prostate biopsy nested within a historical cohort of 10,478 men was conducted to determine whether premalignant prostate telomere length (assessed using a modified qRT-PCR) is associated with prostate cancer risk. Results: Telomere lengths in benign prostate biopsies of cases versus controls were similar (1.46 ± 0.38 vs. 1.45 ± 0.42; P = 0.49). African American (AA) men had significantly shorter telomeres compared with White men (1.51 ± 0.38 vs. 1.63 ± 0.39; P < 0.0001). In race-stratified analyses, increasing telomere length was more strongly associated with prostate cancer risk in White men, wherein those with telomere length in the highest quartile had 1.9-fold greater adjusted risk of prostate cancer compared with men with prostate telomere lengths in the lowest quartile [OR = 1.90; 95% confidence interval (CI) = 1.08–3.36]. Men in the highest telomere length quartile also had a greater risk of aggressive prostate cancer compared with men with telomere lengths in the lowest quartile (OR = 2.78; 95% CI = 1.25–6.19). Conclusions: White men have longer telomeres in benign prostate tissue compared with AA men, and those with the longest telomeres may be at increased risk for prostate cancer, particularly the more aggressive form of the disease. Impact: Race-specific telomere length measures may be an early biomarker of aggressive prostate cancer.

Published

2022

2. A Novel

Author

Judith, Jebastin Thangaiah, Jasmine, Vickery, Wasim, Selwanes, Eman, Al-Haddad, Kyle D, Perry, Nallasivam, Palanisamy, Janet M, Poulik, Sean R, Williamson, Dhananjay A, Chitale, and Bhaig M, Shehata

Subjects

Collagen Type I, alpha 1 Chain, Male, Child, Preschool, Calcium-Binding Proteins, Myofibroma, Skull Neoplasms, Trans-Activators, Humans, Oncogene Fusion, Fasciitis, Collagen Type I

Abstract

Cranial fasciitis is an uncommon benign fibroblastic tumor, generally histologically identical to nodular fasciitis. It develops almost exclusively in children. Cranial fasciitis manifests clinically as a painless rapidly growing solitary nodule in the head and neck area, frequently eroding the underlying bone. Thus, this entity is often confused with aggressive lesions such as sarcomas, both clinically and radiologically. Histopathologic examination is essential to differentiate between cranial fasciitis and fibrohistiocytic or even sarcomatous lesions observed in children. In this article, we present a case of cranial fasciitis with intracranial extension in a 2-year-old boy. Although

Published

2020

3. Breast and prostate cancers harbor common somatic copy number alterations that consistently differ by race and are associated with survival

Author

Benjamin A. Rybicki, Yalei Chen, Indrani Datta, Kanika Taneja, Nilesh S. Gupta, Albert M. Levin, Dhananjay A Chitale, Jia Li, Melissa Davis, Craig G. Rogers, Lisa A. Newman, Sudha M. Sadasivan, Ruicong She, and Pamela L. Paris

Subjects

0301 basic medicine, Oncology, Male, lcsh:Internal medicine, medicine.medical_specialty, Race, lcsh:QH426-470, DNA Copy Number Variations, Somatic cell, Genetic ancestry, Breast Neoplasms, SCNA, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Breast cancer, Prostate, Internal medicine, Genetics, Biomarkers, Tumor, Ethnicity, Medicine, Cluster Analysis, Humans, Clinical significance, lcsh:RC31-1245, Genetics (clinical), business.industry, Gene Expression Profiling, Racial Groups, Chromosome, Prostatic Neoplasms, Genomics, medicine.disease, Prognosis, Human genetics, Gene Expression Regulation, Neoplastic, Survival Rate, lcsh:Genetics, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, SCNAs, Female, business, Research Article

Abstract

Background Pan-cancer studies of somatic copy number alterations (SCNAs) have demonstrated common SCNA patterns across cancer types, but despite demonstrable differences in aggressiveness of some cancers by race, pan-cancer SCNA variation by race has not been explored. This study investigated a) racial differences in SCNAs in both breast and prostate cancer, b) the degree to which they are shared across cancers, and c) the impact of these shared, race-differentiated SCNAs on cancer survival. Methods Utilizing data from The Cancer Genome Atlas (TCGA), SCNAs were identified using GISTIC 2.0, and in each tumor type, differences in SCNA magnitude between African Americans (AA) and European Americans (EA) were tested using linear regression. Unsupervised hierarchical clustering of the copy number of genes residing in race-differentiated SCNAs shared between tumor types was used to identify SCNA-defined patient groups, and Cox proportional hazards regression was used to test for association between those groups and overall/progression-free survival (PFS). Results We identified SCNAs that differed by race in breast (n = 58 SCNAs; permutation p − 4) and prostate tumors (n = 78 SCNAs; permutation p = 0.006). Six race-differentiated SCNAs common to breast and prostate found at chromosomes 5q11.2-q14.1, 5q15-q21.1, 8q21.11-q21.13, 8q21.3-q24.3, 11q22.3, and 13q12.3-q21.3 had consistent differences by race across both tumor types, and all six were of higher magnitude in AAs, with the chromosome 8q regions being the only amplifications. Higher magnitude copy number differences in AAs were also identified at two of these race-differentiated SCNAs in two additional hormonally-driven tumor types: endometrial (8q21.3-q24.3 and 13q12.3-q21.3) and ovarian (13q12.3-q21.3) cancers. Race differentiated SCNA-defined patient groups were significantly associated with survival differences in both cancer types, and these groups also differentiated within triple negative breast cancers based on PFS. While the frequency of the SCNA-defined patient groups differed by race, their effects on survival did not. Conclusions This study identified race-differentiated SCNAs shared by two related cancers. The association of SCNA-defined patient groups with survival demonstrates the clinical significance of combinations of these race-differentiated genomic aberrations, and the higher frequency of these alterations in AA relative to EA patients may explain racial disparities in risk of aggressive breast and prostate cancer.

Published

2019

4. Clonal evaluation of prostate cancer molecular heterogeneity in biopsy samples by dual immunohistochemistry and dual RNA in situ hybridization

Author

Pavithra, Dedigama-Arachchige, Shannon, Carskadon, Jia, Li, Ian, Loveless, Mohamed, Alhamar, James O, Peabody, Hans, Stricker, Dhananjay A, Chitale, Craig G, Rogers, Mani, Menon, Nilesh S, Gupta, Tarek A, Bismar, Sean R, Williamson, and Nallasivam, Palanisamy

Subjects

Adult, Aged, 80 and over, Male, Proto-Oncogene Proteins c-ets, Biopsy, Prostate, Prostatic Neoplasms, Middle Aged, Immunohistochemistry, DNA-Binding Proteins, Transcriptional Regulator ERG, Trypsin Inhibitor, Kazal Pancreatic, Humans, In Situ Hybridization, Aged, Transcription Factors

Abstract

Prostate cancer is frequently multifocal. Although there may be morphological variation, the genetic underpinnings of each tumor are not clearly understood. To assess the inter and intra tumor molecular heterogeneity in prostate biopsy samples, we developed a combined immunohistochemistry and RNA in situ hybridization method for the simultaneous evaluation of ERG, SPINK1, ETV1, and ETV4. Screening of 601 biopsy cores from 120 consecutive patients revealed multiple alterations in a mutually exclusive manner in 37% of patients, suggesting multifocal tumors with considerable genetic differences. Furthermore, the incidence of molecular heterogeneity was higher in African Americans patients compared with Caucasian American patients. About 47% of the biopsy cores with discontinuous tumor foci showed clonal differences with distinct molecular aberrations. ERG positivity occurred in low-grade cancer, whereas ETV4 expression was observed mostly in high-grade cancer. Further studies revealed correlation between the incidence of molecular markers and clinical and pathologic findings, suggesting potential implications for diagnostic pathology practice, such as defining dominant tumor nodules and discriminating juxtaposed but molecularly different tumors of different grade patterns.

Published

2019

5. Methylation in benign prostate and risk of disease progression in men subsequently diagnosed with prostate cancer

Author

Benjamin A, Rybicki, Andrew, Rundle, Oleksandr N, Kryvenko, Nicoleta, Mitrache, Kieu C, Do, Michelle, Jankowski, Dhananjay A, Chitale, Sheri, Trudeau, Steven A, Belinsky, and Deliang, Tang

Subjects

Male, Risk, Carcinogenesis, Prostate, Prostatic Hyperplasia, Prostatic Neoplasms, Kaplan-Meier Estimate, Sequence Analysis, DNA, DNA Methylation, Middle Aged, Article, Cohort Studies, Gene Expression Regulation, Neoplastic, Disease Progression, Humans, Aged, Proportional Hazards Models

Abstract

In DNA from prostate tumors, methylation patterns in gene promoter regions can be a biomarker for disease progression. It remains unclear whether methylation patterns in benign prostate tissue--prior to malignant transformation--may provide similar prognostic information. To determine whether early methylation events predict prostate cancer outcomes, we evaluated histologically benign prostate specimens from 353 men who eventually developed prostate cancer and received "definitive" treatment [radical prostatectomy (58%) or radiation therapy (42%)]. Cases were drawn from a large hospital-based cohort of men with benign prostate biopsy specimens collected between 1990 and 2002. Risk of disease progression associated with methylation was estimated using time-to-event analyses. Average follow-up was over 5 years; biochemical recurrence (BCR) occurred in 91 cases (26%). In White men, methylation of the APC gene was associated with increased risk of BCR, even after adjusting for standard clinical risk factors for prostate cancer progression (adjusted hazard ratio (aHR) = 2.26; 95%CI 1.23-4.16). APC methylation was most strongly associated with a significant increased risk of BCR in White men with low prostate specific antigen at cohort entry (HR = 3.66; 95%CI 1.51-8.85). In additional stratified analyses, we found that methylation of the RARB gene significantly increased risk of BCR in African American cases who demonstrated methylation of at least one of the other four genes under study (HR = 3.80; 95%CI 1.07-13.53). These findings may have implications in the early identification of aggressive prostate cancer as well as reducing unnecessary medical procedures and emotional distress for men who present with markers of indolent disease.

Published

2015