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HOXB13 mutations and binding partners in prostate development and cancer:Function,clinical significance, and future directions 被引量:2

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摘要 The recent and exciting discovery of germline HOXB13 mutations in familial prostate cancer has brought HOX signaling to the forefront of prostate cancer research.An enhanced understanding of HOX signaling,and the co-factors regulating HOX protein specificity and transcriptional regulation,has the high potential to elucidate novel approaches to prevent,diagnose,stage,and treat prostate cancer.Toward our understanding of HOX biology in prostate development and prostate cancer,basic research in developmental model systems as well as other tumor sites provides a mechanistic framework to inform future studies in prostate biology.Here we describe our current understanding of HOX signaling in genitourinary development and cancer,current clinical data of HOXB13 mutations in multiple cancers including prostate cancer,and the role of HOX protein co-factors in development and cancer.These data highlight numerous gaps in our understanding of HOX function in the prostate,and present numerous potentially impactful mechanistic and clinical opportunities for future investigation.
出处 《Genes & Diseases》 SCIE 2017年第2期75-87,共13页 基因与疾病(英文)
基金 DOD PCRP PC130587(Vander Griend) NWU/UC/NSUHS Prostate SPORE(P50 CA180995)the University of Chicago Comprehensive Cancer Center(UCCCC) especially the Cancer Center Support Grant(P30CA014599) H.Brechka and C.Van Opstall were supported by the Cancer Biology Training Grant(T32 CA009594) R.Bhanvadia is supported by a University of Chicago Pritzker School of Medicine Fellowship.
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