a Team "Myeloid Malignancies and Multiple Myeloma" , Université Côte d'Azur, Inserm U1065/C3M , Nice , France.
Autophagy. 2019 May;15(5):927-929. doi: 10.1080/15548627.2019.1586259. Epub 2019 Mar 1.
Chaperone-mediated autophagy (CMA) is a selective form of autophagy that allows the elimination and recycling of cytosolic proteins endowed with a KFERQ-like motif into the lysosome. During this process, the proteins to be degraded are recognized by cellular chaperones such as HSC70 and presented to the CMA receptor LAMP2A, which then translocate them into lysosomes for degradation. In this punctum, we discuss the mechanisms underlying the response and resistance to Azacitidine (Aza) in MDS/AML cell lines and bone marrow CD34+ blasts from MDS/AML patients. We show that treatment of MDS/AML cell lines and bone marrow samples from MDS/AML patients with Aza triggers loss of LAMP2 expression leading to CMA defects. LAMP2 deficiency is responsible for CMA defects, Aza resistance and hypersensitivity to lysosome and autophagy inhibitors. Low levels of LAMP2 expression in CD34+ blasts from MDS/AML patients correlate with an absence of response to Aza and are associated to a pejorative overall survival. We propose that CD34+/LAMP2Low patients at diagnosis or who become CD34+/LAMP2Low during the course of treatment with Aza could receive an autophagy inhibitor available in the clinic.
伴侣蛋白介导的自噬(CMA)是一种选择性的自噬形式,允许具有 KFERQ 样基序的细胞质蛋白被消除和再循环到溶酶体中。在这个过程中,待降解的蛋白质被细胞伴侣如 HSC70 识别,并呈递给 CMA 受体 LAMP2A,然后将它们转运到溶酶体中进行降解。在这一点上,我们讨论了 MDS/AML 细胞系和 MDS/AML 患者骨髓 CD34+ blasts 对阿扎胞苷(Aza)的反应和耐药性的机制。我们表明,用 Aza 处理 MDS/AML 细胞系和 MDS/AML 患者的骨髓样本会触发 LAMP2 表达的丧失,导致 CMA 缺陷。LAMP2 缺陷是 CMA 缺陷、Aza 耐药性和对溶酶体和自噬抑制剂的敏感性增加的原因。MDS/AML 患者骨髓 CD34+blasts 中低水平的 LAMP2 表达与对 Aza 无反应相关,并与不良的总生存相关。我们提出,在诊断时或在接受 Aza 治疗过程中成为 CD34+/LAMP2Low 的患者可以接受临床可用的自噬抑制剂。
