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Comparative analysis of 1152 African-American and European-American men with prostate cancer identifies distinct genomic and immunological differences

Ahmed Mohsen; Alger Jordan; Alshalalfa Mohammed; Awasthi Shivanshu; Beamer Matthew; Beksac Alp Tuna; Bradley Randy; Carmen Darrell J.; Chakravarty Dimple; Davicioni Elai; Deane Leslie A.; Den Robert B.; Falagario Ugo G.; Feng Felix Y.; Greenberger Mark D.; Hwang Jonathan; Khan Irtaza; Liu Yang; Mahal Brandon; Merisaari Harri; Mohamed Nihal; Nair Sujit S.; Nguyen Paul L.; Rayford Walter; Schaeffer Edward M.; Spratt Daniel E.; Stamatakis Lambros; Tewari Ashutosh K.; Watson Justin M.; Weil Rachel; Yadav Kamlesh K.; Yamoah Kosj

Comparative analysis of 1152 African-American and European-American men with prostate cancer identifies distinct genomic and immunological differences

Ahmed Mohsen
Alger Jordan
Alshalalfa Mohammed
Awasthi Shivanshu
Beamer Matthew
Beksac Alp Tuna
Bradley Randy
Carmen Darrell J.
Chakravarty Dimple
Davicioni Elai
Deane Leslie A.
Den Robert B.
Falagario Ugo G.
Feng Felix Y.
Greenberger Mark D.
Hwang Jonathan
Khan Irtaza
Liu Yang
Mahal Brandon
Merisaari Harri
Mohamed Nihal
Nair Sujit S.
Nguyen Paul L.
Rayford Walter
Schaeffer Edward M.
Spratt Daniel E.
Stamatakis Lambros
Tewari Ashutosh K.
Watson Justin M.
Weil Rachel
Yadav Kamlesh K.
Yamoah Kosj
Katso/Avaa
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NATURE RESEARCH
doi:10.1038/s42003-021-02140-y
URI
https://www.nature.com/articles/s42003-021-02140-y
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Julkaisun pysyvä osoite on:
https://urn.fi/URN:NBN:fi-fe2021093049086
Tiivistelmä

Racial disparities in prostate cancer have not been well characterized on a genomic level. Here we show the results of a multi-institutional retrospective analysis of 1,152 patients (596 African-American men (AAM) and 556 European-American men (EAM)) who underwent radical prostatectomy. Comparative analyses between the race groups were conducted at the clinical, genomic, pathway, molecular subtype, and prognostic levels. The EAM group had increased ERG (P<0.001) and ETS (P=0.02) expression, decreased SPINK1 expression (P<0.001), and basal-like (P<0.001) molecular subtypes. After adjusting for confounders, the AAM group was associated with higher expression of CRYBB2, GSTM3, and inflammation genes (IL33, IFNG, CCL4, CD3, ICOSLG), and lower expression of mismatch repair genes (MSH2, MSH6) (p<0.001 for all). At the pathway level, the AAM group had higher expression of genes sets related to the immune response, apoptosis, hypoxia, and reactive oxygen species. EAM group was associated with higher levels of fatty acid metabolism, DNA repair, and WNT/beta-catenin signaling. Based on cell lines data, AAM were predicted to have higher potential response to DNA damage. In conclusion, biological characteristics of prostate tumor were substantially different in AAM when compared to EAM. Walter Rayford, Alp Tuna Beksac et al. investigated gene expression alterations in African-American and European-American men who underwent radical prostatectomy for prostate cancer. The observed differences include higher expression of inflammation genes and lower expression of mismatch repair genes in African-American men.

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