雌激素和抗雌激素通过 GPER1-PRKACA-CMA 通路稳定 MORC2,促进乳腺癌细胞的增殖和内分泌耐药。
Stabilization of MORC2 by estrogen and antiestrogens through GPER1- PRKACA-CMA pathway contributes to estrogen-induced proliferation and endocrine resistance of breast cancer cells.
机构信息
Shanghai Cancer Center and Institutes of Biomedical Sciences, Shanghai Medical College, Fudan University , Shanghai, China.
Department of Breast Surgery, Shanghai Cancer Center, Shanghai Medical College, Fudan University , Shanghai, China.
出版信息
Autophagy. 2020 Jun;16(6):1061-1076. doi: 10.1080/15548627.2019.1659609. Epub 2019 Sep 6.
UNLABELLED
Aberrant activation of estrogen signaling through three ESR (estrogen receptor) subtypes, termed ESR1/ERα, ESR2/ERβ, and GPER1 (G protein-coupled estrogen receptor 1), is implicated in breast cancer pathogenesis and progression. Antiestrogens tamoxifen (TAM) and fulvestrant (FUL) are effective for treatment of ESR1-positive breast tumors, but development of resistance represents a major clinical challenge. However, the molecular mechanisms behind these events remain largely unknown. Here, we report that 17β-estradiol (E2), TAM, and FUL stabilize MORC2 (MORC family CW-type zinc finger 2), an emerging oncoprotein in human cancer, in a GPER1-dependent manner. Mechanistically, GPER1 activates PRKACA (protein kinase cAMP-activated catalytic subunit alpha), which in turn phosphorylates MORC2 at threonine 582 (T582). Phosphorylated MORC2 decreases its interaction with HSPA8 (heat shock protein family A [Hsp70] member 8) and LAMP2A (lysosomal associated membrane protein 2A), two core components of the chaperone-mediated autophagy (CMA) machinery, thus protecting MORC2 from lysosomal degradation by CMA. Functionally, knockdown of attenuates E2-induced cell proliferation and enhances cellular sensitivity to TAM and FUL. Moreover, introduction of wild-type MORC2, but not its phosphorylation-lacking mutant (T582A), in MORC2-depleted cells restores resistance to antiestrogens. Clinically, the phosphorylation levels of MORC2 at T582 are elevated in breast tumors from patients undergoing recurrence after TAM treatment. Together, these findings delineate a phosphorylation-dependent mechanism for MORC2 stabilization in response to estrogen and antiestrogens via blocking CMA-mediated lysosomal degradation and uncover a dual role for MORC2 in both estrogen-induced proliferation and resistance to antiestrogen therapies of breast cancer cells.
ABBREVIATIONS
4-OHT: 4-hydroxytamoxifen; Baf A1: bafilomycin A; CMA: chaperone-mediated autophagy; E2: 17β-estradiol; ESR: estrogen receptor; FUL: fulvestrant; GPER1: G protein-coupled estrogen receptor 1; HSPA8: heat shock protein family A (Hsp70) member 8; LAMP2A: lysosomal associated membrane protein 2A; MORC2: MORC family CW-type zinc finger 2; PRKACA: protein kinase cAMP-activated catalytic subunit alpha; TAM: tamoxifen; VCL: vinculin.
未加标签
雌激素信号的异常激活通过三种 ESR(雌激素受体)亚型,称为 ESR1/ERα、ESR2/ERβ 和 GPER1(G 蛋白偶联雌激素受体 1),与乳腺癌的发病机制和进展有关。他莫昔芬(TAM)和氟维司群(FUL)等抗雌激素药物对治疗 ESR1 阳性乳腺癌有效,但耐药性的发展仍是一个主要的临床挑战。然而,这些事件背后的分子机制在很大程度上仍不清楚。在这里,我们报告 17β-雌二醇(E2)、TAM 和 FUL 以 GPER1 依赖的方式稳定 MORC2(MORC 家族 CW 型锌指 2),这是人类癌症中的一种新兴癌蛋白。在机制上,GPER1 激活 PRKACA(蛋白激酶 cAMP 激活的催化亚单位α),后者反过来使 MORC2 在苏氨酸 582(T582)磷酸化。磷酸化的 MORC2 减少与 HSPA8(热休克蛋白家族 A [Hsp70]成员 8)和 LAMP2A(溶酶体相关膜蛋白 2A)的相互作用,这两种是伴侣介导的自噬(CMA)机制的核心成分,从而防止 MORC2 通过 CMA 进行溶酶体降解。在功能上,敲低 会减弱 E2 诱导的细胞增殖,并增强细胞对 TAM 和 FUL 的敏感性。此外,在 MORC2 耗尽的细胞中引入野生型 MORC2,但不是其缺乏磷酸化的突变体(T582A),可恢复对抗雌激素的耐药性。临床上,在接受 TAM 治疗后复发的患者的乳腺癌肿瘤中,MORC2 的 T582 磷酸化水平升高。总之,这些发现描绘了雌激素和抗雌激素通过阻断 CMA 介导的溶酶体降解来稳定 MORC2 的一种依赖于磷酸化的机制,并揭示了 MORC2 在雌激素诱导的增殖和乳腺癌细胞对抗雌激素治疗的耐药性中具有双重作用。
缩写
4-OHT:4-羟基他莫昔芬;Baf A1:巴佛洛霉素 A;CMA:伴侣介导的自噬;E2:17β-雌二醇;ESR:雌激素受体;FUL:氟维司群;GPER1:G 蛋白偶联雌激素受体 1;HSPA8:热休克蛋白家族 A(Hsp70)成员 8;LAMP2A:溶酶体相关膜蛋白 2A;MORC2:MORC 家族 CW 型锌指 2;PRKACA:蛋白激酶 cAMP 激活的催化亚单位α;TAM:他莫昔芬;VCL: vinculin。
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