The interaction between androgen receptor and semenogelin I : a synthetic LxxLL peptide antagonist inhibits the growth of prostate cancer cells
Menée sur des lignées cellulaires de cancer de la prostate, cette étude montre qu'un peptide synthétique, comportant le motif d'acides aminés LxxLL de la séménogéline I (une protéine séminale) et antagoniste du récepteur androgénique, peut inhiber la croissance des cellules cancéreuses
Background : We previously demonstrated that a seminal plasma protein, semenogelin I (SgI), functioned as an androgen receptor (AR) coactivator. Meanwhile, several short sequence motifs in AR coregulators, such as LxxLL (L=leucine), have been shown to mediate specific interactions with AR. Methods : We investigated the role of the LxxLL motif within SgI in the interactions with AR and cell growth in prostate cancer lines in vitro. Results : A full-length SgI with mutations in the motif (i.e., LxxAA; A=alanine) failed to significantly increase cell proliferation/migration as well as androgen-mediated AR transcription. Co-immunoprecipitation showed no physical interactions between AR and the mutant SgI. In addition, transfection of an 18-amino acid peptide of SgI containing LxxLL, but not LxxAA, resulted in considerable reduction in cell growth and prostate-specific antigen expression in LNCaP and C4-2 lines. Conclusions : The LxxLL motif of SgI could be a novel therapeutic target for both androgen-sensitive and castration-resistant prostate cancers.