84 results on '"Mansukhani, Mahesh"'
Search Results
2. Benchmarking bioinformatics approaches for tumour mutational burden evaluation from a large cancer panel against whole-exome sequencing.
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Jiuhong Pang, Hongai Xia, Shijun Mi, Wen Zhang, Pendrick, Danielle, Freeman, Christopher, Fernandes, Helen, Mansukhani, Mahesh, and Hsiao, Susan J.
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PROGRAMMED cell death 1 receptors ,FALSE positive error ,TUMORS ,INSTITUTIONAL review boards - Published
- 2023
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3. Papillary Intralymphatic Angioendothelioma in a Child With PIK3CA -Related Overgrowth Spectrum: Implication of PI3K Pathway in the Vascular Tumorigenesis.
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Debelenko, Larisa, Mansukhani, Mahesh M., and Remotti, Fabrizio
- Abstract
Papillary intralymphatic angioendothelioma (PILA) is an extremely rare vascular tumor and its pathogenesis is unknown. Phosphatidylinositol-4,5-bisphosphate 3-kinase catalytic subunit alpha (PIK3CA)-related overgrowth spectrum (PROS) is a heterogeneous group of disorders caused by mosaicism for activating mutations of PIK3CA and characterized by asymmetric overgrowth, skeletal anomalies, skin lesions, and vascular malformations. An association between PILA and PROS has not been known. We report a case of PILA involving the spleen of a young girl with the clinical and molecular diagnosis of PROS. Sequencing of the patient's germ-line DNA detected a pathogenic PIK3CA variant c.1357G>A in 10.6% of alleles. Splenectomy revealed a 4-cm tumor composed of ectatic lymphatics with intraluminal papillary projections, consistent with PILA. The tumor cells showed immunohistochemical expression of CD31, CD34, ERG, FLI-1, PROX1, and caldesmon, while D2-40 was negative. The latter may suggest that the tumor derived from an endothelial precursor arrested in the final steps of lymphothelial differentiation, in keeping with the known role of the PIK3CA -governed molecular pathway in the progression of vascular progenitors to mature endothelial cells. The data implicates PIK3CA in the pathogenesis of PILA and broadens the spectrum of phenotypic expressions of PROS. [ABSTRACT FROM AUTHOR]
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- 2023
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4. Pineal region ganglioglioma: A neoplasm with a bimodal age distribution.
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Al-Dalahmah, Osama A., Wang, Linda, Hsiao, Susan J., Chun-Chieh Lin, Mansukhani, Mahesh M., Canoll, Peter, Bruce, Jeffrey N., and Zanazzi, George
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- 2022
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5. Clinical exome sequencing for inherited retinal degenerations at a tertiary care center.
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Ganapathi, Mythily, Thomas-Wilson, Amanda, Buchovecky, Christie, Dharmadhikari, Avinash, Barua, Subit, Lee, Winston, Ruan, Merry Z. C., Soucy, Megan, Ragi, Sara, Tanaka, Joy, Clark, Lorraine N., Naini, Ali B., Liao, Jun, Mansukhani, Mahesh, Tsang, Stephen, and Jobanputra, Vaidehi
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Inherited retinal degenerations are clinically and genetically heterogeneous diseases characterized by progressive deterioration of vision. This study aimed at assessing the diagnostic yield of exome sequencing (ES) for an unselected cohort of individuals with hereditary retinal disorders. It is a retrospective study of 357 unrelated affected individuals, diagnosed with retinal disorders who underwent clinical ES. Variants from ES were filtered, prioritized, and classified using the ACMG recommendations. Clinical diagnosis of the individuals included rod-cone dystrophy (60%), macular dystrophy (20%), cone-rod dystrophy (9%), cone dystrophy (4%) and other phenotypes (7%). Majority of the cases (74%) were singletons and 6% were trios. A confirmed molecular diagnosis was obtained in 24% of cases. In 6% of cases, two pathogenic variants were identified with phase unknown, bringing the potential molecular diagnostic rate to ~ 30%. Including the variants of uncertain significance (VUS), potentially significant findings were reported in 57% of cases. Among cases with a confirmed molecular diagnosis, variants in EYS, ABCA4, USH2A, KIZ, CERKL, DHDDS, PROM1, NR2E3, CNGB1, ABCC6, PRPH2, RHO, PRPF31, PRPF8, SNRNP200, RP1, CHM, RPGR were identified in more than one affected individual. Our results support the utility of clinical ES in the diagnosis of genetically heterogeneous retinal disorders. [ABSTRACT FROM AUTHOR]
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- 2022
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6. Pineal region ganglioglioma: A neoplasm with a bimodal age distribution.
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Al-Dalahmah, Osama A., Wang, Linda, Hsiao, Susan J., Chun-Chieh Lin, Mansukhani, Mahesh M., Canoll, Peter, Bruce, Jeffrey N., and Zanazzi, George
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AGE distribution ,NATURAL history ,MITOGEN-activated protein kinases ,TUMORS in children ,YOUNG adults - Abstract
Background: Gangliogliomas arise very rarely in the pineal region, where their natural histories and pathologic features are poorly understood. Case Description: In this report, we describe a 36-year-old woman who presented with a seizure followed by worsening headache, dizziness, confusion, and intermittent left facial numbness over the next few weeks. A head CT scan showed a partially calcified pineal region mass with hydrocephalus. After an endoscopic third ventriculostomy, the patient underwent a resection of the tumor that contained dysplastic ganglion cells and piloid glial cells. Molecular profiling of this CNS WHO Grade 1 ganglioglioma revealed polysomies of chromosomes 7 and 9, and a BUB1 variant of uncertain significance, without known MAP kinase pathway alterations. From a review of the literature, we found two distinct age distributions for pineal ganglioglioma, with modes at 1 and 36 years of age. Conclusion: Although very rare, this tumor should be considered in the differential diagnosis of pineal region tumors in children and young adults. [ABSTRACT FROM AUTHOR]
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- 2022
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7. ZTTK syndrome: Clinical and molecular findings of 15 cases and a review of the literature.
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Kushary, Sulagna Tina, Revah‐Politi, Anya, Barua, Subit, Ganapathi, Mythily, Accogli, Andrea, Aggarwal, Vimla, Brunetti‐Pierri, Nicola, Cappuccio, Gerarda, Capra, Valeria, Fagerberg, Christina R., Gazdagh, Gabriella, Guzman, Edwin, Hadonou, Medard, Harrison, Victoria, Havelund, Kathrine, Iancu, Daniela, Kraus, Alison, Lippa, Natalie C., Mansukhani, Mahesh, and McBrian, Danielle
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Zhu‐Tokita‐Takenouchi‐Kim (ZTTK) syndrome is caused by de novo loss‐of‐function variants in the SON gene (MIM #617140). This multisystemic disorder is characterized by intellectual disability, seizures, abnormal brain imaging, variable dysmorphic features, and various congenital anomalies. The wide application and increasing accessibility of whole exome sequencing (WES) has helped to identify new cases of ZTTK syndrome over the last few years. To date, there have been approximately 45 cases reported in the literature. Here, we describe 15 additional individuals with variants in the SON gene, including those with missense variants bringing the total number of known cases to 60. We have reviewed the clinical and molecular data of these new cases and all previously reported cases to further delineate the most common as well as emerging clinical findings related to this syndrome. Furthermore, we aim to delineate any genotype–phenotype correlations specifically for a recurring pathogenic four base pair deletion (c.5753_5756del) along with discussing the impact of missense variants seen in the SON gene. [ABSTRACT FROM AUTHOR]
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- 2021
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8. Whole-Exome Sequencing Identifies a Novel POLG Frameshift Variant in an Adult Patient Presenting with Progressive External Ophthalmoplegia and Mitochondrial DNA Depletion.
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Kurtz, Justin, Fernandes Jr, Joseph Americo, Mansukhani, Mahesh, Copeland, William C., and Naini, Ali B.
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MITOCHONDRIAL DNA ,NUCLEAR DNA ,EYE paralysis ,MUSCLE weakness ,MITOCHONDRIA ,HETEROZYGOSITY - Abstract
Mitochondrial DNA (mtDNA) depletion syndromes are a group of autosomal recessive disorders associated with a spectrum of clinical diseases, which include progressive external ophthalmoplegia (PEO). They are caused by variants in nuclear DNA (nDNA) encoded genes, and the gene that encodes for mtDNA polymerase gamma (POLG) is commonly involved. A splice-site mutation in POLG, c.3104+3A > T, was previously identified in three families with findings of PEO, and studies demonstrated this variant to result in skipping of exon 19. Here, we report a 57-year-old female who presented with ophthalmoplegia, ptosis, muscle weakness, and exercise intolerance with a subsequent muscle biopsy demonstrating mitochondrial myopathy on histopathologic evaluation and multiple mtDNA deletions by southern blot analysis. Whole-exome sequencing identified the previously characterized c. 3104+3A > T splice-site mutation in compound heterozygosity with a novel frameshift variant, p.Gly23Serfs ∗ 236 (c.67_88del). mtDNA copy number analysis performed on the patient's muscle showed mtDNA depletion, as expected in a patient with biallelic pathogenic mutations in POLG. This is the first reported case with POLG p.Gly23Serfs ∗ 236, discovered in a patient presenting with features of PEO. [ABSTRACT FROM AUTHOR]
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- 2021
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9. Rosette-Forming Glioneuronal Tumor in the Pineal Region: A Series of 6 Cases and Literature Review.
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Lin, Chun-Chieh, Mansukhani, Mahesh M, Bruce, Jeffrey N, Canoll, Peter, and Zanazzi, George
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- 2021
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10. Immunophenotypic Spectrum and Genomic Landscape of Refractory Celiac Disease Type II.
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Soderquist, Craig R., Lewis, Suzanne K., Gru, Alejandro A., Vlad, George, Williams, Eli S., Susan Hsiao, Mansukhani, Mahesh M., Park, David C., Bacchi, Carlos E., Alobeid, Bachir, Green, Peter H., and Bhagat, Govind
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- 2021
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11. Predictive testing for neurodegenerative diseases in the age of next‐generation sequencing.
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Goldman, Jill, Xie, Shanghong, Green, Dina, Naini, Ali, Mansukhani, Mahesh M., and Marder, Karen
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The availability and cost of next‐generation sequencing (NSG) now allow testing large numbers of genes simultaneously. However, the gold standard for predictive testing has been to test only for a known family mutation or confirmed family disease. The goal of this study was to investigate the psychological impact of predictive testing for autosomal dominant neurodegenerative diseases without a known family mutation using next‐generation sequencing panels compared to single‐gene testing of a known family mutation. Fourteen individuals from families with a known mutation and 10 individuals with unknown family mutations participated. Participants completed questionnaires on demographics, genetic knowledge, and psychological measures of anxiety, depression, perceived personal control, rumination, and intolerance to uncertainty at baseline and 1 and 6 months after receiving results. Decision regret was measured 1 and 6 months after receiving results. Participants completed a modified Huntington disease genetic testing protocol with genetic counseling and neurological and psychological evaluation. Genetic testing of either the known family mutation or an NGS panel of neurodegenerative disease genes was performed. Semi‐structured interviews were performed at 6 months post‐results about their experience. Two‐sample t tests were performed on data collected at each time point to identify significant between‐group differences in demographic variables, baseline psychological scores, and baseline genetic knowledge scores. Within‐group change over time was assessed by a mixed‐effects model. Results of this study indicate that NGS panels for predictive testing for neurodegenerative disease are safe and beneficial to participants when performed within a modified HD protocol. Though significant differences in psychological outcomes were found, these differences may have been driven by genetic results and baseline psychological differences between individuals within the groups. Participants did not regret their decision to test and were largely pleased with the testing protocol. [ABSTRACT FROM AUTHOR]
- Published
- 2021
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12. Field-deployable, rapid diagnostic testing of saliva for SARS-CoV-2.
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Wei, Shan, Suryawanshi, Hemant, Djandji, Alexandre, Kohl, Esther, Morgan, Stephanie, Hod, Eldad A., Whittier, Susan, Roth, Kevin, Yeh, Raymond, Alejaldre, Juan Carlos, Fleck, Elaine, Ferrara, Stephen, Hercz, Daniel, Andrews, David, Lee, Lilly, Hendershot, Kristopher A., Goldstein, Joshua, Suh, Yousin, Mansukhani, Mahesh, and Williams, Zev
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SALIVA ,COVID-19 testing ,POLYMERASE chain reaction ,LABORATORIES ,CLINICAL trials - Abstract
To safely re-open economies and prevent future outbreaks, rapid, frequent, point-of-need, SARS-CoV-2 diagnostic testing is necessary. However, existing field-deployable COVID-19 testing methods require the use of uncomfortable swabs and trained providers in PPE, while saliva-based methods must be transported to high complexity laboratories for testing. Here, we report the development and clinical validation of High-Performance Loop-mediated isothermal Amplification (HP-LAMP), a rapid, saliva-based, SARS-CoV-2 test with a limit of detection of 1.4 copies of virus per µl of saliva and a sensitivity and specificity with clinical samples of > 96%, on par with traditional RT-PCR based methods using swabs, but can deliver results using only a single fluid transfer step and simple heat block. Testing of 120 patient samples in 40 pools comprised of 5 patient samples each with either all negative or a single positive patient sample was 100% accurate. Thus, HP-LAMP may enable rapid and accurate results in the field using saliva, without need of a high-complexity laboratory. [ABSTRACT FROM AUTHOR]
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- 2021
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13. Direct diagnostic testing of SARS-CoV-2 without the need for prior RNA extraction.
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Wei, Shan, Kohl, Esther, Djandji, Alexandre, Morgan, Stephanie, Whittier, Susan, Mansukhani, Mahesh, Hod, Eldad, D'Alton, Mary, Suh, Yousin, and Williams, Zev
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COVID-19 pandemic ,NUCLEIC acid isolation methods ,GENE amplification ,DETECTION limit ,SURGICAL swabs - Abstract
The COVID-19 pandemic has resulted in an urgent need for a rapid, point of care diagnostic testing that could be rapidly scaled on a worldwide level. We developed and tested a highly sensitive and robust assay based on reverse transcription loop mediated isothermal amplification (RT-LAMP) that uses readily available reagents and a simple heat block using contrived spike-in and actual clinical samples. RT-LAMP testing on RNA-spiked samples showed a limit of detection (LoD) of 2.5 copies/μl of viral transport media. RT-LAMP testing directly on clinical nasopharyngeal swab samples in viral transport media had an 85% positive percentage agreement (PPA) (17/20), and 100% negative percentage agreement (NPV) and delivered results in 30 min. Our optimized RT-LAMP based testing method is a scalable system that is sufficiently sensitive and robust to test for SARS-CoV-2 directly on clinical nasopharyngeal swab samples in viral transport media in 30 min at the point of care without the need for specialized or proprietary equipment or reagents. This cost-effective and efficient one-step testing method can be readily available for COVID-19 testing world-wide, especially in resource poor settings. [ABSTRACT FROM AUTHOR]
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- 2021
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14. Compound heterozygous inheritance of two novel COQ2 variants results in familial coenzyme Q deficiency.
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Abdelhakim, Aliaa H., Dharmadhikari, Avinash V., Ragi, Sara D., de Carvalho, Jose Ronaldo Lima, Xu, Christine L., Thomas, Amanda L., Buchovecky, Christie M., Mansukhani, Mahesh M., Naini, Ali B., Liao, Jun, Jobanputra, Vaidehi, Maumenee, Irene H., Tsang, Stephen H., and de Carvalho, Jose Ronaldo Lima Jr
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RECESSIVE genes ,LAURENCE-Moon-Biedl syndrome ,BIOSYNTHESIS ,ELECTRORETINOGRAPHY ,UBIQUINONES ,RARE diseases - Abstract
Background: Primary coenzyme Q10 deficiency is a rare disease that results in diverse and variable clinical manifestations. Nephropathy, myopathy and neurologic involvement are commonly associated, however retinopathy has also been observed with certain pathogenic variants of genes in the coenzyme Q biosynthesis pathway. In this report, we describe a novel presentation of the disease that includes nephropathy and retinopathy without neurological involvement, and which is the result of a compound heterozygous state arising from the inheritance of two recessive potentially pathogenic variants, previously not described.Materials and Methods: Retrospective report, with complete ophthalmic examination, multimodal imaging, electroretinography, and whole exome sequencing performed on a family with three affected siblings.Results: We show that affected individuals in the described family inherited two heterozygous variants of the COQ2 gene, resulting in a frameshift variant in one allele, and a predicted deleterious missense variant in the second allele (c.288dupC,p.(Ala97Argfs*56) and c.376C > G,p.(Arg126Gly) respectively). Electroretinography results were consistent with rod-cone dystrophy in the affected individuals. All affected individuals in the family exhibited the characteristic retinopathy as well as end-stage nephropathy, without evidence of any neurological involvement.Conclusions: We identified two novel compound heterozygous variants of the COQ2 gene that result in primary coenzyme Q deficiency. Targeted sequencing of coenzyme Q biosynthetic pathway genes may be useful in diagnosing oculorenal clinical presentations syndromes not explained by more well known syndromes (e.g., Senior-Loken and Bardet-Biedl syndromes). [ABSTRACT FROM AUTHOR]- Published
- 2020
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15. Diffuse midline glioma with novel, potentially targetable, FGFR2-VPS35 fusion.
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Zanazzi, George, Liechty, Benjamin L., Pendrick, Danielle, Krasnozhen-Ratush, Olga, Snuderl, Matija, Allen, Jeffrey C., Garvin, James H., Mansukhani, Mahesh M., Roth, Kevin A., and Hsiao, Susan J.
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GLIOMAS ,FIBROBLAST growth factor 2 ,FLUORESCENCE in situ hybridization ,TRANSCRIPTOMES ,FIBROBLAST growth factors - Abstract
We report a case of a slow-growing, diffuse, infiltrating glioma in the right brainstem of a 9-yr-old boy. The tumor was negative by immunohistochemical staining for histone H3 K27M, BRAFV600E, and IDH1 R132H mutations. Fluorescence in situ hybridization did not reveal a BRAF duplication. Genomic profiling of the tumor, by DNA methyl-ation array and cancer whole-exome and transcriptome sequencing, was performed. This analysis showed copy-number alterations, including gains of several chromosomes. In addition, a novel fusion involving the first 17 exons of FGFR2 fused to exon 2 of VPS35 was identified. This novel fusion is predicted to result in activation of fibroblast growth factor receptor (FGFR) signaling and is potentially targetable using FGFR inhibitors. Thistumorex-pands the spectrum of pediatric diffuse gliomas. [ABSTRACT FROM AUTHOR]
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- 2020
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16. Clinical Utilization, Utility, and Reimbursement for Expanded Genomic Panel Testing in Adult Oncology.
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Hsiao, Susan J., Sireci, Anthony N., Pendrick, Danielle, Freeman, Christopher, Fernandes, Helen, Schwartz, Gary K., Henick, Brian S., Mansukhani, Mahesh M., Roth, Kevin A., Carvajal, Richard D., and Oberg, Jennifer A.
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REIMBURSEMENT ,ACADEMIC medical centers ,NUCLEOTIDE sequencing ,INDIVIDUALIZED medicine - Abstract
PURPOSE: The routine use of large next-generation sequencing (NGS) pan-cancer panels is required to identify the increasing number of, but often uncommon, actionable alterations to guide therapy. Inconsistent coverage and variable payment is hindering NGS adoption into clinical practice. A review of test utilization, clinical utility, coverage, and reimbursement was conducted in a cohort of patients diagnosed with high-risk cancer who received pan-cancer panel testing as part of their clinical care. MATERIALS AND METHODS: The Columbia Combined Cancer Panel (CCCP), a 467-gene panel designed to detect DNA variations in solid and liquid tumors, was performed in the Laboratory of Personalized Genomic Medicine at Columbia University Irving Medical Center. Utilization was characterized at test order. Results were reviewed by a molecular pathologist, followed by a multidisciplinary molecular tumor board where clinical utility was classified by consensus. Reimbursement was reviewed after payers provided final coverage decisions. RESULTS: NGS was performed on 359 high-risk tumors from 349 patients. Reimbursement data were available for 246 cases. The most common reason providers ordered CCCP testing was for patients diagnosed with a treatment-resistant or recurrent tumor (n = 214; 61%). Findings were clinically impactful for 229 cases (64%). Molecular alterations that may inform future therapy in the event of progression or relapse were found in 42% of cases, and a targeted therapy was initiated in 23 cases (6.6%). The majority of tests were denied coverage by payers (n = 190; 77%). On average, insurers reimbursed 10.75% of the total NGS service charge. CONCLUSION: CCCP testing identified clinically impactful alterations in 64% of cases. Limited coverage and low reimbursement remain barriers, and broader reimbursement policies are needed to adopt pan-cancer NGS testing that benefits patients into clinical practice. [ABSTRACT FROM AUTHOR]
- Published
- 2020
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17. Spontaneous Regression and Complete Response to Immune Checkpoint Blockade in a Case of High-Grade Neuroendocrine Carcinoma.
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Raufi, Alexander G., May, Michael, Greendyk, Richard A., Iuga, Alina, Ahmed, Firas, Mansukhani, Mahesh, and Manji, Gulam A.
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SPONTANEOUS cancer regression ,CARCINOMA ,TUMOR antigens ,IMMUNE response ,SKIN cancer ,IMMUNE checkpoint inhibitors - Published
- 2020
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18. Refractory celiac disease type II: An atypical case highlighting limitations of the current classification system.
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Soderquist, Craig R., Hsiao, Susan, Mansukhani, Mahesh M., Alobeid, Bachir, Green, Peter H., and Bhagat, Govind
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T-cell lymphoma ,SYMPTOMS ,CLASSIFICATION ,GENE rearrangement - Abstract
Refractory celiac disease (RCD) is a rare condition associated with high morbidity that develops in individuals with celiac disease. It is known to be biologically heterogeneous, and currently two types are recognized based on immunophenotypic and molecular features, type I (RCD I) and type II (RCD II). Differentiating between RCD I and RCD II is critical, as patients with RCD II have substantially worse outcomes and a high risk of developing enteropathy-associated T-cell lymphoma. However, the current RCD classification is limited in scope, and atypical presentations and immunophenotypes are not recognized at present. Herein, we describe a unique case of RCD II with atypical clinical (primarily neurologic manifestations and lack of significant gastrointestinal symptoms), histopathologic (no villous atrophy), immunophenotypic (virtual absence of cytoplasmic CD3 expression), and molecular features (absence of clonal TR rearrangement and identification of pathogenic STAT3 and KMT2D mutations). This case highlights limitations of the current RCD classification system and the utility of next generation sequencing (NGS) studies in the diagnostic workup of RCD. Future algorithms need to recognize extraintestinal manifestations and incorporate atypical histopathologic and immunophenotypic features, as well as results of NGS analysis for RCD II classification. [ABSTRACT FROM AUTHOR]
- Published
- 2020
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19. Assay Complementarity to Overcome False-Negative Testing for Microsatellite Instability/Mismatch Repair Deficiency: A Pembrolizumab-Sensitive Intimal Sarcoma.
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Henick, Brian S., Ingham, Matthew, Shirazi, Maryam, Marboe, Charles, Turk, Andrew, Hsiao, Susan, and Mansukhani, Mahesh M.
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HEREDITARY nonpolyposis colorectal cancer ,MICROSATELLITE repeats ,SARCOMA ,PROGRAMMED death-ligand 1 - Abstract
A 58-year-old woman was diagnosed with a T4N1, moderately differentiated rectal adenocarcinoma 10 years before presentation to our center; the disease was treated with chemoradiation followed by low-anterior resection and 3 months of adjuvant capecitabine plus oxaliplatin. Lancet Oncol; 18: 1493-1501, 2017 9 Wilky BA, Trucco MM, Subhawong TK, et al: Axitinib plus pembrolizumab in patients with advanced sarcomas including alveolar soft-part sarcoma: A single-centre, single-arm, phase 2 trial. [Extracted from the article]
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- 2020
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20. Microsatellite instability detection using a large next-generation sequencing cancer panel across diverse tumour types.
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Jiuhong Pang, Gindin, Tatyana, Mansukhani, Mahesh, Fernandes, Helen, and Hsiao, Susan
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NUCLEOTIDE sequencing ,TUMORS ,CANCER ,DNA mismatch repair ,HEREDITARY nonpolyposis colorectal cancer ,GASTROINTESTINAL cancer - Published
- 2020
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21. Cytogenetic analysis of 130 renal oncocytomas identify three distinct and mutually exclusive diagnostic classes of chromosome aberrations.
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Anderson, Christopher B., Lipsky, Michael, Nandula, Subhadra V., Freeman, Christopher E., Matthews, Thomas, Walsh, Caitlin E., Li, Gen, Szabolcs, Matthias, Mansukhani, Mahesh M., McKiernan, James M., and Murty, Vundavalli V.
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- 2020
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22. SETD2 Mutation in an Aggressive Optic Nerve Glioma.
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Campbell, Ashley A., Gartrell-Corrado, Robyn D., Mansukhani, Mahesh, Zanazzi, George, Canoll, Peter, Garvin, James H., and Kazim, Michael
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- 2020
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23. Clonal T cell receptor gene rearrangements in coeliac disease: implications for diagnosing refractory coeliac disease.
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Hussein, Shafinaz, Gindin, Tatyana, Lagana, Stephen M., Arguelles-Grande, Carolina, Krishnareddy, Suneeta, Alobeid, Bachir, Lewis, Suzanne K., Mansukhani, Mahesh M., Green, Peter H. R., and Bhagat, Govind
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CELIAC disease complications ,GENE rearrangement ,CELIAC disease ,PHENOTYPES ,T cell receptors ,SMALL intestine ,BIOPSY - Published
- 2018
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24. You have free access to this contentTargeted next generation sequencing of breast implant-associated anaplastic large cell lymphoma reveals mutations in JAK/STAT signalling pathway genes, TP53 and DNMT3A.
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Di Napoli, Arianna, Jain, Preti, Duranti, Enrico, Margolskee, Elizabeth, Arancio, Walter, Facchetti, Fabio, Alobeid, Bachir, Santanelli di Pompeo, Fabio, Mansukhani, Mahesh, and Bhagat, Govind
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BREAST implants ,ANAPLASTIC lymphoma kinase ,LYMPHOCYTES ,BIOMARKERS ,GENETIC mutation - Abstract
The article focuses on next generation sequencing of breast implant associated anaplastic large cell lymphoma (BI-ALCL) which reveals mutations in JAK/STAT signalling pathway genes, TP53 and DNMT3A. It mentions BI-ALCL is characterized by the presence of CD30 with atypical lymphocytes frequently confined to the peri-implant seroma fluid. It also mentions identification of biomarkers that enable disease prognostication and optimal treatment.
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- 2018
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25. Prevalence and Physical Distribution of SRY in the Gonads of a Woman with Turner Syndrome: Phenotypic Presentation, Tubal Formation, and Malignancy Risk.
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Baer, Tamar G., Freeman, Christopher E., Cujar, Claudia, Mansukhani, Mahesh, Singh, Bahadur, Chen, Xiaowei, Abellar, Rosanna, Oberfield, Sharon E., and Levy, Brynn
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SRY gene ,GONADS ,TURNER'S syndrome - Abstract
Although monosomy X is the most common karyotype in patients with Turner syndrome, the presence of Y chromosome material has been observed in about 10% of patients. Y chromosome material in patients with Turner syndrome poses an increased risk of gonadoblastoma and malignant transformation. We report a woman with a diagnosis of Turner syndrome at 12 years of age, without signs of virilization and karyotype reported as 46,X,del(X)(q13). At 26 years, cytogenetic studies indicated the patient to be mosaic for monosomy X and a cell line that contained a duplicated Yq chromosome. Bilateral gonadectomy was performed and revealed streak gonads, without evidence of gonadoblastoma. Histological analysis showed ovarian stromal cells with few primordial tubal structures. FISH performed on streak gonadal tissue showed a heterogeneous distribution of SRY, with exclusive localization to the primordial tubal structures. DNA extraction from the gonadal tissue showed a 6.5% prevalence of SRY by microarray analysis, contrasting the 86% prevalence in the peripheral blood sample. This indicates that the overall gonadal sex appears to be determined by the majority gonosome complement in gonadal tissue in cases of sex chromosome mosaicism. This case also raises questions regarding malignancy risk associated with Y prevalence and tubal structures in gonadal tissue. [ABSTRACT FROM AUTHOR]
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- 2017
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26. Use of Oncogenic Driver Mutations in Staging of Multiple Primary Lung Carcinomas: A Single-Center Experience.
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Asmar, Ramsey, Sonett, Joshua R., Singh, Gopal, Mansukhani, Mahesh M., and Borczuk, Alain C.
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- 2017
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27. Identification of recurrent mutational events in anorectal melanoma.
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Yang, Hui Min, Hsiao, Susan J, Schaeffer, David F, Lai, Chi, Remotti, Helen E, Horst, David, Mansukhani, Mahesh M, and Horst, Basil A
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- 2017
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28. A case study of an integrative genomic and experimental therapeutic approach for rare tumors: identification of vulnerabilities in a pediatric poorly differentiated carcinoma.
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Dela Cruz, Filemon S., Diolaiti, Daniel, Turk, Andrew T., Rainey, Allison R., Ambesi-Impiombato, Alberto, Andrews, Stuart J., Mansukhani, Mahesh M., Nagy, Peter L., Alvarez, Mariano J., Califano, Andrea, Forouhar, Farhad, Modzelewski, Beata, Mitchell, Chelsey M., Yamashiro, Darrell J., Marks, Lianna J., Glade Bender, Julia L., and Kung, Andrew L.
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TUMOR treatment ,EXPERIMENTAL design ,MOLECULAR structure ,CARCINOMA ,GENOMES ,THERAPEUTICS - Abstract
Background: Precision medicine approaches are ideally suited for rare tumors where comprehensive characterization may have diagnostic, prognostic, and therapeutic value. We describe the clinical case and molecular characterization of an adolescent with metastatic poorly differentiated carcinoma (PDC). Given the rarity and poor prognosis associated with PDC in children, we utilized genomic analysis and preclinical models to validate oncogenic drivers and identify molecular vulnerabilities. Methods: We utilized whole exome sequencing (WES) and transcriptome analysis to identify germline and somatic alterations in the patient’s tumor. In silico and in vitro studies were used to determine the functional consequences of genomic alterations. Primary tumor was used to generate a patient-derived xenograft (PDX) model, which was used for in vivo assessment of predicted therapeutic options. Results: WES revealed a novel germline frameshift variant (p.E1554fs) in APC, establishing a diagnosis of Gardner syndrome, along with a somatic nonsense (p.R790*) APC mutation in the tumor. Somatic mutations in TP53, MAX, BRAF, ROS1, and RPTOR were also identified and transcriptome and immunohistochemical analyses suggested hyperactivation of the Wnt/ß-catenin and AKT/mTOR pathways. In silico and biochemical assays demonstrated that the MAX p.R60Q and BRAF p.K483E mutations were activating mutations, whereas the ROS1 and RPTOR mutations were of lower utility for therapeutic targeting. Utilizing a patient-specific PDX model, we demonstrated in vivo activity of mTOR inhibition with temsirolimus and partial response to inhibition of MEK. Conclusions: This clinical case illustrates the depth of investigation necessary to fully characterize the functional significance of the breadth of alterations identified through genomic analysis. [ABSTRACT FROM AUTHOR]
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- 2016
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29. Impact of the Arg 16 allele of the B2AR gene on the effect of withdrawal of LABA in patients with moderate to severe asthma.
- Author
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Slankard, Marjorie, Michelis, Mary Ann, Mansukhani, Mahesh, McGoey, Barbara, Paige, Amy, Andrews, Howard, Lederer, David, Canfield, Stephen, and DiMango, Emily
- Subjects
ASTHMA treatment ,ADRENERGIC beta agonists ,GENETIC polymorphisms ,ADRENERGIC receptors ,GENOTYPES - Abstract
Introduction: Long-acting beta agonists (LABAs) are effective for controlling asthma, however questions about their safety have led to concerns over use. Genetic polymorphisms at the 16 amino acid position of the beta-2 adrenergic receptor gene (B2AR) may be associated with increased risk.Methods: A randomized, double blind study was conducted in patients with moderate to severe asthma being treated with combined inhaled corticosteroids/LABA (ICS/LABA), comparing the effect of LABA continuation versus withdrawal on asthma outcomes among patients stratified by B2AR genotype (Arg/Arg vs. Gly/Gly at the 16th amino acid position).Results: 67 participants (31 Arg/Arg, 36 Gly/Gly) were randomized to receive fluticasone alone (F) or continue combined fluticasone/salmeterol (F/S) after a run-in period on F/S. Among Gly/Gly subjects, those in the F/S treatment group showed improvement in AM PEFR (+ 8.4 L/s) whereas those receiving F alone experienced a reduction in AM PEFR over the study period (−14.4 L/s), (p= 0.06). There was no significant difference in morning peak expiratory flow rate (AM PEFR) in Arg/Arg participants randomized to receive F/S (−15.7L) vs F alone (−5.6 L/s) (p= 0.61). There was no significant difference in exacerbations in the Arg/Arg subjects treated with F/S compared with those treated with F (p= 0.65).Conclusions: Withdrawal of LABA therapy in asthmatics with the Arg/Arg genotype at the 16th amino acid position of B2AR did not lead to significant improvement in AM PEFR. LABA withdrawal in the Gly/Gly genotype however led to a borderline significant decline in AM PEFR. [ABSTRACT FROM AUTHOR]
- Published
- 2016
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30. Epigenetic Inactivation of TRAIL Decoy Receptors at 8p12-21.3 Commonly Deleted Region Confers Sensitivity to Apo2L/TRAIL-Cisplatin Combination Therapy in Cervical Cancer.
- Author
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Narayan, Gopeshwar, Xie, Dongxu, Ishdorj, Ganchimeg, Scotto, Luigi, Mansukhani, Mahesh, Pothuri, Bhavana, Wright, Jason D., Kaufmann, Andreas M., Schneider, Achim, Arias‐Pulido, Hugo, and Murty, Vundavalli V.
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- 2016
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31. The role of clinical genomic testing in diagnosis and discovery of pathogenic mutations.
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Nagy, Peter L and Mansukhani, Mahesh
- Abstract
Next-generation sequencing in clinical practice allows for a critical review of the literature to evaluate disease relatedness of specific genes and pathogenicity of individual mutations, while providing an important discovery tool for new disease genes and disease-causing mutations. Data obtained from large panels, whole exome or whole genome sequencing, performed for constitutional or cancer cases, need to be managed in a transparent, yet powerful analytical framework. Assessment of reported pathogenic potential of a variant or disease association of a gene requires careful consideration of population allele frequency, variant data from parents, and precise, yet concise phenotypic description of the entire family and other individuals or families that have the same variant. The full potential for discovery can only be realized if there is data sharing between clinicians performing the interpretation worldwide and structural biologists, analytical chemists and cell biologists interested and knowledgeable of the structure and function of the genes involved. [ABSTRACT FROM PUBLISHER]
- Published
- 2015
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32. Practical diagnostic approaches to composite plasma cell neoplasm and low grade B-cell lymphoma/clonal infiltrates in the bone marrow.
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Hussein, Shafinaz, Gill, Kamraan, Baer, Lea N., Hoehn, Daniela, Mansukhani, Mahesh, Jobanputra, Vaidehi, Bhagat, Govind, and Alobeid, Bachir
- Abstract
Composite plasma cell neoplasm (PCN) and low grade B-cell lymphoma (B-NHL) in the bone marrow are uncommon and raise the differential diagnosis of B-NHL with plasmacytic differentiation and PCN with lymphoplasmacytic morphology. This can be a challenging differential diagnosis, and the distinctions are important because of differences in management. We report five cases of composite PCN with B-NHL or clonal B-cell infiltrates involving the bone marrow. By using multiple different diagnostic modalities, including immunophenotyping by flow cytometry and immunohistochemistry, cytogenetic analysis and IGH gene rearrangement studies by polymerase chain reaction, we were able to distinguish two distinct clonally unrelated neoplasms in all cases. We describe the utility and pitfalls of these different diagnostic modalities. Flow cytometric analysis with a panel of antibodies that includes CD19, CD56, CD138, CD45 and other aberrant markers commonly expressed by PCN will allow identification of clonally unrelated PCN and B-NHL in a composite neoplasm, and distinguish them from B-NHL with plasmacytic differentiation and PCN with lymphoplasmacytic morphology. Cytogenetic and molecular analyses can give false-negative or false-positive results. In summary, a multimodal approach utilizing these different tools, including clinical data, should be used to arrive at the correct diagnosis. Copyright © 2014 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]
- Published
- 2015
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33. Cytomorphological features of ALK-positive lung adenocarcinomas: Psammoma bodies and signet ring cells.
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Pareja, Fresia, Crapanzano, John P., Mansukhani, Mahesh M., Bulman, William A., and Saqi, Anjali
- Abstract
BACKGROUND Correlation between histology and genotype has been described in lung adenocarcinomas. For example, studies have demonstrated that adenocarcinomas with an anaplastic lymphoma kinase ( ALK) gene rearrangement may have mucinous features. The objective of the current study was to determine whether a similar association can be identified in cytological specimens. METHODS A retrospective search for ALK-rearranged cytopathology (CP) and surgical pathology (SP) lung carcinomas was conducted. Additional ALK-negative (-) lung adenocarcinomas served as controls. For CP and SP cases, the clinical data (i.e., age, sex, and smoking history), architecture, nuclear features, presence of mucin-containing cells (including signet ring cells), and any additional salient characteristics were evaluated. RESULTS The search yielded 20 ALK-positive (+) adenocarcinomas. Compared with patients with ALK(-) lung adenocarcinomas (33 patients; 12 with epidermal growth factor receptor [ EGFR]-mutation, 11 with Kristen rat sarcoma [ KRAS]-mutation, and 10 wild-type adenocarcinomas), patients with ALK(+) adenocarcinoma presented at a younger age; and there was no correlation noted with sex or smoking status. The most common histological pattern in SP was papillary/micropapillary. Mucinous features were associated with ALK rearrangement in SP specimens. Signet ring cells and psammoma bodies were evident in and significantly associated with ALK(+) SP and CP specimens. However, psammoma bodies were observed in rare adenocarcinomas with an EGFR mutation. Both the ALK(+) and ALK(−) groups had mostly high nuclear grade. CONCLUSIONS Salient features, including signet ring cells and psammoma bodies, were found to be significantly associated with ALK(+) lung adenocarcinomas and are identifiable on CP specimens. Recognizing these may be especially helpful in the molecular triage of scant CP samples. Cancer (Cancer Cytopathol) 2014. © 2014 American Cancer Society. Cancer (Cancer Cytopathol) 2015;123:162-170. © 2014 American Cancer Society. [ABSTRACT FROM AUTHOR]
- Published
- 2015
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34. Bladder cancers arise from distinct urothelial sub-populations.
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Van Batavia, Jason, Yamany, Tammer, Molotkov, Andrei, Dan, Hanbin, Mansukhani, Mahesh, Batourina, Ekaterina, Schneider, Kerry, Oyon, Daniel, Dunlop, Mark, Wu, Xue-Ru, Cordon-Cardo, Carlos, and Mendelsohn, Cathy
- Subjects
BLADDER cancer ,TRANSITIONAL cell carcinoma ,URINARY organ cancer ,BASAL cell carcinoma ,SKIN cancer - Abstract
Bladder cancer is the sixth most common cancer in humans. This heterogeneous set of lesions including urothelial carcinoma (Uca) and squamous cell carcinoma (SCC) arise from the urothelium, a stratified epithelium composed of K5-expressing basal cells, intermediate cells and umbrella cells. Superficial Uca lesions are morphologically distinct and exhibit different clinical behaviours: carcinoma in situ (CIS) is a flat aggressive lesion, whereas papillary carcinomas are generally low-grade and non-invasive. Whether these distinct characteristics reflect different cell types of origin is unknown. Here we show using lineage tracing in a murine model of carcinogenesis that intermediate cells give rise primarily to papillary lesions, whereas K5-basal cells are likely progenitors of CIS, muscle-invasive lesions and SCC depending on the genetic background. Our results provide a cellular and genetic basis for the diversity in bladder cancer lesions and provide a possible explanation for their clinical and morphological differences. [ABSTRACT FROM AUTHOR]
- Published
- 2014
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35. Validity and Reliability of Using a Self-Lavaging Device for Cytology and HPV Testing for Cervical Cancer Screening: Findings from a Pilot Study.
- Author
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Jones, Heidi E., Mansukhani, Mahesh M., Tong, Guo-Xia, and Westhoff, Carolyn L.
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TEST validity ,RELIABILITY (Personality trait) ,CERVICAL cancer ,CYTOLOGY ,PAPILLOMAVIRUSES ,COLPOSCOPY ,HISTOLOGY - Abstract
: Self-sampling could increase cervical cancer screening uptake. While methods have been identified for human papillomavirus (HPV) testing, to date, self-sampling has not provided adequate specimens for cytology. We piloted the validity and reliability of using a self-lavaging device for cervical cytology and HPV testing. We enrolled 198 women in New York City in 2008–2009 from three ambulatory clinics where they received cervical cancer screening. All were asked to use the Delphi Screener™ to self-lavage 1–3 months after clinician-collected index cytological smear (100 normal; 98 abnormal). Women with abnormal cytology results from either specimen underwent colposcopy; 10 women with normal results from both specimens also underwent colposcopy. We calculated sensitivity of self-collected cytology to detect histologically confirmed high grade lesions (cervical intraepithelial neoplasia, CIN, 2+); specificity for histology-negative (CIN 1 or lower), paired cytology negative, or a third cytology negative; and kappa for paired results. One hundred and ninety-seven (99.5%) women self-collected a lavage. Seventy-five percent had moderate to excellent cellularity, two specimens were unsatisfactory for cytology. Seven of 167 (4%) women with definitive results had CIN2+; one had normal and six abnormal cytology results with the self-lavage (sensitivity = 86%, 95% Confidence Interval, CI: 42, 100). The kappa for paired cytology was low (0.36; 95% CI: 0.25, 0.47) primarily due to clinician specimens with atypical squamous cells of undetermined significance (ASC-US) and low grade squamous intraepithelial lesion (LSIL) coded as normal using Screener specimens. However, three cases of HSIL were coded as ASC-US and one as normal using Screener specimens. Seventy-three women had paired high-risk HPV tests with a kappa of 0.66 (95% CI: 0.49, 0.84). Based on these preliminary findings, a larger study to estimate the performance of the Screener for co-testing cytology and HPV or for HPV testing with cytology triage is warranted. Trial Registration: ClinicalTrials.gov NCT00702208 [ABSTRACT FROM AUTHOR]
- Published
- 2013
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36. Peripheral T-cell lymphoma emerging in a patient with aggressive polymyositis: molecular evidence for neoplastic transformation of an oligoclonal T-cell infiltrate.
- Author
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Tsankova, Nadejda, Bevan, Carolyn, Jobanputra, Vaidehi, Ko, Yen, Mayer, Elizabeth, Lefkowitch, Jay, Mansukhani, Mahesh, Rowland, Lewis, Bhagat, Govind, and Tanji, Kurenai
- Subjects
T-cell lymphoma ,POLYMYOSITIS ,IMMUNOHISTOCHEMISTRY ,SINGLE nucleotide polymorphisms ,GENOMICS - Abstract
We report a rare case of peripheral T-cell lymphoma arising in a 52-year-old man with biopsy-proven aggressive polymyositis, who had cardiac involvement, progressive bulbar symptoms, and died 11 months post diagnosis due to multiorgan failure. Using a multimodality approach including immunohistochemistry, genome-wide single nucleotide polymorphism (SNP)-array analysis, and high-throughput sequencing of the complementary determining region 3 (CDR3) of T-cell receptor beta (TCRβ) genes, our study demonstrates a molecular link between polymyositis and T-cell lymphoma, and provides evidence of the rapid and possibly late occurrence of genomic instability during neoplastic transformation of an oligoclonal T-cell population. Immunohistochemical analysis revealed loss of CD5, CD7, and CD8 antigen expression in autopsy tissue samples, as well as the occurrence of aberrant CD56 expression, not seen in pre-mortem biopsies, supporting the emergence of a neoplastic T-cell population. Multiplex polymerase chain reaction and next-generation sequencing of the TCRβ CDR3 region displayed two unique T-cell clones in both the diagnostic biopsy confirming polymyositis and the autopsy muscle tissue exhibiting T-cell lymphoma, linking the two pathological processes. SNP-array analysis revealed complex genomic abnormalities at autopsy but not in the pre-mortem muscle biopsies displaying polymyositis, confirming malignant transformation of the oligoclonal T-cell infiltrate. Our findings raise the possibility that clinically aggressive polymyositis might represent a preneoplastic condition in some instances, similar to certain other autoimmune and inflammatory disorders. [ABSTRACT FROM AUTHOR]
- Published
- 2013
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37. Thymidylate synthase expression and molecular alterations in adenosquamous carcinoma of the lung.
- Author
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Shu, Catherine, Cheng, Haiying, Wang, Antai, Mansukhani, Mahesh M, Powell, Charles A, Halmos, Balazs, and Borczuk, Alain C
- Published
- 2013
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38. Mutation in an mtDNA Protein-Coding Gene: Prenatal Diagnosis Aided by Fetal Muscle Biopsy.
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Shanske, Sara, Naini, Ali, Chmait, Ramen H., Akman, Hasan O., Mansukhani, Mahesh, Lu, Jiesheng, Hirano, Michio, and DiMauro, Salvatore
- Subjects
PRENATAL diagnosis ,GENETIC code ,ADENOSINE triphosphatase ,MITOCHONDRIAL DNA ,FETAL tissues ,GENETIC disorder diagnosis - Abstract
Prenatal diagnosis of disorders due to mitochondrial DNA (mtDNA) tRNA gene mutations is problematic. Experience in families harboring the protein-coding ATPase 6 m.8993T>G mutation suggests that the mutant load is homogeneous in different tissues, thus allowing prenatal diagnosis. We have encountered a novel protein-coding gene mutation, m.10198C>T in MT-ND3. A baby girl homoplasmic for this mutation died at 3 months after severe psychomotor regression and respiratory arrest. The mother had no detectable mutation in accessible tissues. The product of a second pregnancy showed only wild-type mt genomes in amniocytes, chorionic villi, and biopsied fetal muscle. This second girl is now 18 months old and healthy. Our observations support the concept that the pathogenic mutation in this patient appeared de novo and that fetal muscle biopsy is a useful aide in prenatal diagnosis. [ABSTRACT FROM AUTHOR]
- Published
- 2013
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39. Real-time PCR-based analysis of BRAF V600E mutation in low and intermediate grade lymphomas confirms frequent occurrence in hairy cell leukaemia.
- Author
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Ewalt, Mark, Nandula, Subhadra, Phillips, Adrienne, Alobeid, Bachir, Murty, Vundavalli V., Mansukhani, Mahesh M., and Bhagat, Govind
- Abstract
Hairy cell leukaemia (HCL) is a rare type of B-cell non-Hodgkin lymphoma (B-NHL), which is not known to be associated with any characteristic recurrent karyotypic abnormality. A recent study that used massively parallel whole exome sequencing identified an activating V600E mutation in BRAF, which appeared specific for HCL. Here, we confirm the specificity of BRAF V600E for HCL among low and intermediate grade B-NHL and describe a real-time polymerase chain reaction method for detecting this mutation in cases with low tumour burden. The V600E mutation does not appear to be associated with microsatellite instability, unlike the case in colorectal cancer. Thus, in conjunction with prior data, our results suggest incorporation of BRAF V600E mutation analysis in the diagnostic workup of HCL cases. Additionally, targeting the Ras-Raf-Mek-Erk-Map kinase pathway should be investigated as a potential therapeutic strategy for patients with this disease. Copyright © 2011 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]
- Published
- 2012
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40. A comparison of the outcomes of neoadjuvant and adjuvant chemotherapy for clinical T2-T4aN0-N2M0 bladder cancer.
- Author
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Wosnitzer, Matthew S., Hruby, Gregory W., Murphy, Alana M., Barlow, Lamont J., Cordon-Cardo, Carlos, Mansukhani, Mahesh, Petrylak, Daniel P., Benson, Mitchell C., and McKiernan, James M.
- Subjects
DRUG therapy ,BLADDER cancer ,CISPLATIN ,PATIENTS ,CANCER - Abstract
BACKGROUND: Despite evidence supporting perioperative chemotherapy, few randomized studies compare neoadjuvant and adjuvant chemotherapy for bladder cancer. Consequently, the standard of care regarding the timing of chemotherapy for locally advanced bladder cancer remains controversial. We compared patient outcomes following neoadjuvant or adjuvant systemic chemotherapy for cT2-T4aN0-N2M0 bladder cancer. METHODS: In a retrospective review of a single institutional database from 1988 through 2009, we identified patients receiving neoadjuvant or adjuvant multiagent platinum-based systemic chemotherapy for locally advanced bladder cancer. Survival analysis was performed comparing disease-specific survival (DSS) and overall survival (OS). RESULTS: A total of 146 patients received systemic perioperative chemotherapy (73 neoadjuvant, 73 adjuvant). Of these, 84% (122/146) received cisplatin-based chemotherapy compared with carboplatin-based chemotherapy (24/146, 16.4%). Most patients receiving cisplatin-based chemotherapy were treated with methotrexate/vinblastine/adriamycin/cisplatin (79/122, 64.8%), whereas the remaining patients received gemcitabine/cisplatin (GC) (43/122, 35.2%). In multivariable analysis, there was no significant difference in DSS ( P = .46) or OS ( P = .76) between neoadjuvant or adjuvant chemotherapy groups. There was statistically significant improvement in DSS when patients received neoadjuvant GC rather than adjuvant GC ( P = .049, hazard ratio, 10.6; 95% confidence interval, 1.01-112.2). CONCLUSION: In this study, there was no statistically significant difference in OS and DSS between patients receiving neoadjuvant versus adjuvant systemic platinum-based chemotherapy for locally advanced bladder cancer. In addition, there was no significant difference between neoadjuvant and adjuvant cisplatin- or carboplatin-based chemotherapy. Chemotherapy sequence relative to surgery appeared less important than whether or not a patient actually received perioperative chemotherapy. Cancer 2011;. © 2011 American Cancer Society. [ABSTRACT FROM AUTHOR]
- Published
- 2012
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41. Predictive Value of Microtubule Associated Proteins Tau and Stathmin in Patients With Nonmuscle Invasive Bladder Cancer Receiving Adjuvant Intravesical Taxane Therapy
- Author
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Wosnitzer, Matthew S., Domingo-Domenech, Josep, Castillo-Martin, Mireia, Ritch, Chad, Mansukhani, Mahesh, Petrylack, Daniel P., Benson, Mitchell C., McKiernan, James M., and Cordon-Cardo, Carlos
- Published
- 2011
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42. Cytogenetic abnormalities in reactive lymphoid hyperplasia: byproducts of the germinal centre reaction or indicators of lymphoma?
- Author
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Sevilla, Deborah W., Murty, Vundavalli V., Sun, Xin-Lai, Nandula, Subhadra V., Mansukhani, Mahesh M., Alobeid, Bachir, and Bhagat, Govind
- Abstract
Non-random karyotypic abnormalities associated with non-Hodgkin lymphomas (NHLs) have been described in cases of reactive lymphoid hyperplasia (RLH). However, the frequency and types of cytogenetic aberrations detected and their clinical relevance are unknown. To address these questions, we undertook a retrospective analysis of a large series of RLH diagnosed at our institute over 8 years. Cytogenetic abnormalities were identified in 20 of 116 (17%) cases with informative karyotypes, comprising 14 (70%) structural and 11 (55%) numerical changes. Clonal ( n = 14, 70%) and non-clonal ( n = 6, 30%) abnormalities were observed. Aberrations of chromosome 14 were the most frequent ( n = 8, 42%, 7 represented IgH translocations), followed by chromosome 3 ( n = 4, 3 represented BCL6 translocations), and chromosome 12 ( n = 4). Abnormal karyotypes were most often associated with florid follicular hyperplasia. Isolated lymphoid organ (lymph node, tonsil or spleen) enlargement (12/20, 60%) was more common, no specific etiology was identified in 10/20 (50%) cases and only 1 of 18 patients with clinical follow-up (range 2-107 months, median 60 months) developed lymphoma. In our experience, cytogenetic abnormalities involving loci associated with B-cell NHL are not infrequently detected in RLH. Their occurrence portends low risk for lymphomagenesis, however longer follow-up is prudent to further evaluate the natural history of such cases. Copyright © 2010 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]
- Published
- 2011
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43. Atypical glandular cells (AGC): ThinPrep Imaging System (TIS), manual screening (MS), and correlation with Hybrid Capture 2 (HC2) HPV DNA testing.
- Author
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Sireci, Anthony N., Crapanzano, John P., Mansukhani, Mahesh, Wright, Thomas, Babiac, Anamaria, Erroll, Maria, Vazquez, Madeline, and Saqi, Anjali
- Published
- 2010
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44. Associations between Polycyclic Aromatic Hydrocarbon--Related Exposures and p53 Mutations in Breast Tumors.
- Author
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Mordukhovich, Irina, Rossner, Jr., Pavel, Terry, Mary Beth, Santella, Regina, Yu-Jing Zhang, Hibshoosh, Hanina, Memeo, Lorenzo, Mansukhani, Mahesh, Long, Chang-Min, Garbowski, Gail, Agrawa, Meenakshi, Gaudet, Mia M., Steck, Susan E., Sagiv, Sharon K., Eng, Sybil M., Teitelbaum, Susan L., Neugut, Alfred I., Conway-Dorsey, Kathleen, and Gammon, Marilie D.
- Subjects
POLYCYCLIC aromatic compounds ,HYDROCARBONS ,BREAST cancer ,CARCINOGENS ,GENETIC mutation ,TUMOR suppressor genes ,ETIOLOGY of diseases ,PERIPHERAL circulation ,CELLS ,MEDICAL research - Abstract
Background: Previous studies have suggested that polycyclic aromatic hydrocarbons (PAHs) may be associated with breast cancer. However, the carcinogenicity of PAHs on the human breast remains unclear. Certain carcinogens may be associated with specific mutation patterns in the p53 tumor suppressor gene, thereby contributing information about disease etiology. Objectives: We hypothesized that associations of PAH-related exposures with breast cancer would differ according to tumor p53 mutation status, effect, type, and number. Methods: We examined this possibility in a population-based case-control study using polytomous logistic regression. As previously reported, 151 p53 mutations among 859 tumors were identified using Surveyor nuclease and confirmed by sequencing. Results: We found that participants with p53 mutations were less likely to be exposed to PAHs (assessed by smoking status in 859 cases and 1,556 controls, grilled/smoked meat intake in 822 cases and 1,475 controls, and PAH-DNA adducts in peripheral mononuclear cells in 487 cases and 941 controls) than participants without p53 mutations. For example, active and passive smoking was associated with p53 mutation-negative [odds ratio (OR) = 1.55; 95% confidence interval (CI), 1.11-2.15] but not p53 mutation-positive (OR = 0.77; 95% CI, 0.43-1.38) cancer (ratio of the ORs = 0.50, p < 0.05). However, frameshift mutations, mutation number, G:C→A:T transitions at CpG sites, and insertions/deletions were consistently elevated among exposed subjects. Conclusions: These findings suggest that PAHs may be associated with specific breast tumor p53 mutation subgroups rather than with overall p53 mutations and may also be related to breast cancer through mechanisms other than p53 mutation. [ABSTRACT FROM AUTHOR]
- Published
- 2010
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45. Results of the Southwest Oncology Group phase II evaluation (study S0031) of ZD1839 for advanced transitional cell carcinoma of the urothelium.
- Author
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Petrylak, Daniel P., Tangen, Catherine M., Van Veldhuizen, Peter J., Goodwin, J. Wendall, Twardowski, Przemyslaw W., Atkins, James N., Kakhil, Shaker R., Lange, Marianne K., Mansukhani, Mahesh, and Crawford, E. David
- Subjects
MEDICAL research ,EPIDERMAL growth factor ,CANCER patients ,CANCER chemotherapy ,CEREBROVASCULAR disease ,DISEASE progression ,ONCOLOGY research - Abstract
Study Type – Prognosis (inception cohort) Level of Evidence 1b OBJECTIVE To evaluate the epidermal growth factor receptor (EGFR)-targeted agent ZD1839 in patients who failed one previous chemotherapeutic regimen for metastatic transitional cell carcinoma (TCC), and to correlate patterns of response with the expression of EGFR. PATIENTS AND METHODS Thirty-one patients with metastatic TCC of the urothelial tract were treated with ZD1839 500 mg oral daily. Patients were required to have a pretreatment biopsy to assess EGF expression. RESULTS The median progression-free survival was 2 months, with only two patients (6.5%) surviving past 6 months with no disease progression. Thirty patients were evaluable for toxicity; there was grade 4 cerebrovascular ischaemia and an increase in creatinine level. All patients were evaluable for response, with one confirmed partial response (3%; 95% confidence interval, CI, 0–17%) in a patient with pulmonary metastases. All patients have died, and the estimated median (95% CI) survival is 3 (2–7) months. CONCLUSIONS ZD1839 is ineffective as a second-line agent for urothelial carcinoma. [ABSTRACT FROM AUTHOR]
- Published
- 2010
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46. Collagenous sprue is not always associated with dismal outcomes: a clinicopathological study of 19 patients.
- Author
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Vakiani, Efsevia, Arguelles-Grande, Carolina, Mansukhani, Mahesh M, Lewis, Suzanne K, Rotterdam, Heidrun, Green, Peter H, and Bhagat, Govind
- Published
- 2010
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47. Intraorbital granuloma annulare in an elderly patient.
- Author
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Barrett, Dianne, Petris, Carisa, Garrido Hermosilla, Antonio Manuel, Oktavec, Kathleen, Mansukhani, Mahesh, and Kazim, Michael
- Subjects
OLDER patients ,HISTOLOGY ,ETIOLOGY of diseases - Abstract
Classically, granuloma annulare (GA) is a cutaneous disorder localized to the dorsum of the hands and/or feet in children and young adults. Very rarely it can present on the face and rarer still on periorbital structures such as the eyelid and orbital rim. Diagnosis hinges on clinical presentation and histological features, such as palisading granulomas with central destruction of collagen, presence of mucin and lymphohistiocytic infiltration. The etiology of this condition remains unknown, but may involve a delayed-type hypersensitivity reaction, malignancy and/or infection. Herein is the first reported case of an intraorbital GA in an 86-year-old male patient who presented with right eye proptosis. [ABSTRACT FROM PUBLISHER]
- Published
- 2016
- Full Text
- View/download PDF
48. KHSV− EBV− post-transplant effusion lymphoma with plasmablastic features: variant of primary effusion lymphoma?
- Author
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Lambe, Jennifer S., Oble, Darryl A., Nandula, Subhadra V., Sevilla, Deborah W., Colovai, Adriana I., Mansukhani, Mahesh, Chari, Ajai, Murty, Vundavalli V., Alobeid, Bachir, and Bhagat, Govind
- Abstract
Primary effusion lymphoma (PEL) is a rare type of B-cell non-Hodgkin lymphoma (NHL), which predominantly occurs in HIV-infected individuals, and is pathogenetically linked with Kaposi sarcoma (KS)-associated herpes virus/human herpes virus-8 (KSHV/HHV-8) infection with or without evidence of Epstein-Barr virus (EBV) co-infection. Although uncommon, PELs have been reported in immunocompetent patients and recipients of solid organ allografts. Rare cases of KSHV
− EBV+ post-transplant effusion lymphomas resembling PEL have also been described, as have KSHV− EBV− effusion lymphomas, the latter including those arising in individuals with chronic liver disease. We report a unique KSHV− EBV− post-transplant effusion lymphoma associated with serum paraproteins, occurring in an HIV− individual, which had cytologic features and phenotype similar to PEL, and displayed a complex karyotype including isochromosome 12p and translocation t(8;22), resulting in rearrangement of c-MYC. Copyright © 2009 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]- Published
- 2009
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49. Protocadherin PCDH10, involved in tumor progression, is a frequent and early target of promoter hypermethylation in cervical cancer.
- Author
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Narayan, Gopeshwar, Scotto, Luigi, Neelakantan, Vijayalakshmi, Kottoor, Sherine H., Wong, Ada Ho Yan, Loke, Shee-Loong, Mansukhani, Mahesh, Pothuri, Bhavana, Wright, Jason D., Kaufmann, Andreas M., Schneider, Achim, Arias-Pulido, Hugo, Tao, Qian, and Murty, Vundavalli V.
- Published
- 2009
- Full Text
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50. Mutations in p53, p53 protein overexpression and breast cancer survival.
- Author
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Rossner, Jr., Pavel, Gammon, Marilie D., Yu-Jing Zhang, Terry, Mary Beth, Hibshoosh, Hanina, Memeo, Lorenzo, Mansukhani, Mahesh, Chang-Min Long, Garbowski, Gail, Agrawal, Meenakshi, Kalra, Tara S., Gaudet, Mia M., Teitelbaum, Susan L., Neugut, Alfred I., and Santella, Regina M.
- Subjects
BREAST cancer ,TUMORS ,TUMOR suppressor genes ,PROGESTERONE receptors ,BIOMARKERS - Abstract
p53 is an important tumour suppressor gene that encodes p53 protein, a molecule involved in cell cycle regulation and has been inconsistently linked to breast cancer survival. Using archived tumour tissue from a population-based sample of 859 women diagnosed with breast cancer between 1996 and 1997, we determined p53 mutations in exons 5–8 and p53 protein overexpression. We examined the association of p53 mutations with overexpression and selected tumour clinical parameters. We assessed whether either p53 marker was associated with survival through 2002, adjusting for other tumour markers and prognostic factors. The prevalence of protein overexpression in the tumour was 36% (307/859) and of any p53 mutation was 15% (128/859). p53 overexpression was positively associated with the presence of any p53 mutation (odds ratio [OR]= 2.2, 95% confidence interval [CI]= 1.5–3.2), particularly missense mutations (ER = 7.0, 95% CI = 3.6–13.7). Negative oestrogen and progesterone receptor (ER/PR) status was positively associated with both p53 protein overexpression (= 2.6, 95% CI = 1.7–4.0) and p53 mutation (OR = 3.9, 95% CI = 2.4–6.5). Any p53 mutation and missense mutations, but not p53 protein overexpression, were associated with breast cancer-specific mortality (hazard ratio [HR]= 1.7, 95% CI = 1.0–2.8; HR = 2.0, 95% CI = 1.1–3.6, respectively) and all-cause mortality (HR = 1.5, 95% CI = 1.0–2.4; HR = 2.0, 95% CI = 1.2–3.4, respectively); nonsense mutations were associated only with breast cancer-specific mortality (HR = 3.0, 95% CI = 1.1–8.1). These associations however did not remain after adjusting for ER/PR status. Thus, in this population-based cohort of women with breast cancer, although p53 protein overexpression and p53 mutations were associated with each other, neither independently impacted breast cancer-specific or all-causing mortality, after considering ER/PR status. [ABSTRACT FROM AUTHOR]
- Published
- 2009
- Full Text
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