Authors
Yinxiu Chi, Huixing Pan, Changqi Li, Xianhui Wang
Published in
Clinical laboratory. Volume 72. Issue 6. Jun 01, 2026.
Abstract
The unprocessed precursor of brain-derived neurotrophic factor (BDNF), proBDNF, has emerged as a potential determinant of therapeutic response in prostate cancer. Upon secretion, proBDNF preferentially binds to the co-receptors sortilin and p75NTR, triggering pro-apoptotic or pro-survival cascades, depending on cellular context. ProBDNF engages sortilin/p75NTR to drive castration resistance and metastasis in prostate cancer. High proBDNF/sortilin predicts poor therapy outcome, yet their tissue expression in prostate cancer (PCa) remains unclear.
To evaluate the protein expression levels of proBDNF, sortilin, and p75NTR, we performed immunohistochemical analyses on 18 formalin-fixed paraffin-embedded (FFPE) PCa tissues obtained at radical prostatectomy between 2024 and 2025, together with matched para-carcinoma tissues.
Compared with para-carcinoma tissues, immunohistochemistry in 18 paired specimens showed that pro-BDNF was significantly upregulated in PCa tissues (median IHC score 60.5 (range 57 - 65) vs. 41.5 (40 - 45), p < 0.05). Sortilin expression was also higher in PCa (median 37.0 (35 - 39) vs. 16.5 (15 - 18), p < 0.01); P75 expression remained relatively low in both prostate cancer and adjacent non-cancerous tissues (18.5 (17 - 20) vs. 6.5 (5 - 8), p < 0.05).
These findings suggest a correlation between the expression levels of proBDNF, sortilin, and p75-NTR and the characteristics of PCa. Further investigation into the mechanisms underlying these interactions may provide valuable insights for the development of targeted therapies for PCa.
PMID:
42295304
Bibliographic data and abstract were imported from PubMed on 15 Jun 2026.
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