Literature DB >> 31237441

Clinical implications of mismatch repair deficiency in prostate cancer.

Ramy Sedhom1, Emmanuel S Antonarakis1.   

Abstract

Immune checkpoint blockade holds great promise in the treatment of solid tumors but has not yet been approved for use in advanced prostate cancer. This is largely due to the relatively modest response in clinical trials in unselected patients and the lack of available biomarkers to predict clinical benefit. Germline and somatic mismatch repair (MMR) gene deficiencies are more prevalent than previously thought, especially in the metastatic setting, in patients with high-grade Gleason scores and in patients with variant histologies. An early signal suggests that patients with deficiency in MMR may respond well to immunotherapy. Both germline and somatic genetic testing are recommended, yet questions remain on the best modality for testing given lack of standardization and false-negative results in patients with complex genomic structural rearrangements. Expanded panels, such as next generation sequencing may increase the sensitivity without compromising specificity. Future studies are still needed to explore the relationships of hypermutation, tumor mutational burden, tumor-infiltrating lymphocytes and microsatellite instability-H status as predictors of response to immunotherapy. The drivers of variable response is largely unknown, and a more mature understanding of the mechanisms of resistance in deficiencies in MMR tumors may help to more precisely inform use of immunotherapy in prostate cancer.

Entities:  

Keywords:  germline mutations; immunotherapy; mismatch repair defects; prostate cancer; somatic mutations

Mesh:

Substances:

Year:  2019        PMID: 31237441      PMCID: PMC6714067          DOI: 10.2217/fon-2019-0068

Source DB:  PubMed          Journal:  Future Oncol        ISSN: 1479-6694            Impact factor:   3.404


  89 in total

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3.  Defects of DNA mismatch repair in human prostate cancer.

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Authors:  Abdel-Rahmene Azzouzi; James W F Catto; Ishtiaq Rehman; Stephane Larre; Morgan Roupret; Kenneth M Feeley; Oliver Cussenot; Mark Meuth; Freddie C Hamdy
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Review 8.  The clinical importance and prognostic implications of microsatellite instability in sporadic cancer.

Authors:  D A Lawes; S SenGupta; P B Boulos
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9.  HNPCC versus sporadic microsatellite-unstable colon cancers follow different routes toward loss of HLA class I expression.

Authors:  Jan Willem F Dierssen; Noel F C C de Miranda; Soldano Ferrone; Marjo van Puijenbroek; Cees J Cornelisse; Gert Jan Fleuren; Tom van Wezel; Hans Morreau
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10.  Development of a fluorescent multiplex assay for detection of MSI-High tumors.

Authors:  Jeffery W Bacher; Laura A Flanagan; Regenia L Smalley; Nadine A Nassif; Lawrence J Burgart; Richard B Halberg; Wael M Abdel Megid; Stephen N Thibodeau
Journal:  Dis Markers       Date:  2004       Impact factor: 3.434

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3.  Reduced DNA Repair Capacity in Prostate Cancer Patients: A Phenotypic Approach Using the CometChip.

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Review 4.  Germline Genetics of Prostate Cancer: Prevalence of Risk Variants and Clinical Implications for Disease Management.

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Journal:  Cancers (Basel)       Date:  2021-04-29       Impact factor: 6.639

5.  Genetic Testing and Its Clinical Application in Prostate Cancer Management: Consensus Statements from the Hong Kong Urological Association and Hong Kong Society of Uro-Oncology.

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Review 6.  Microsatellite Instability: From the Implementation of the Detection to a Prognostic and Predictive Role in Cancers.

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  6 in total

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