[No authors listed]
Prostate cancer is closely associated with constitutive transactivation of the androgen receptor (AR) signaling pathway. After treatment with androgenâdeprivation therapy (ADT), the majority of patients develop castrationâresistant prostate cancer within months or years. In order to investigate potential novel therapeutic targets in addition to ADT, the present study examined the regulatory mechanisms of the AR signaling pathway. In the present study, LNCaP cells were metabolicallyâlabeled with AlkâC16, a palmitate probe. In addition, cells were treated with R1881, an androgen, or DMSO. Subsequently, clickâchemistryâbased palmitoylome profiling was performed in LNCaP cells and palmitoylated proteins were compared between cells treated with androgen and untreated cells. Androgen treatment was revealed to significantly increase the palmitoylation level of αâtubulin. In addition, the palmitoylation level of Rasârelated protein Rabâ7a (Rab7a) was enhanced by androgen treatment. Palmitoylation of αâtubulin and Rab7a were essential for cell proliferation. Notably, in the supernatant of LNCaP cells, the palmitoylation level of αâtubulin was also increased following androgen treatment. Palmitoylation of αâtubulin may provide a new potential target for the treatment of prostate cancer. In addition, the high level of αâtubulin palmitoylation in the supernatant may represent a biomarker for earlyâstage prostate cancer.
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