Cuervo Ana Maria, Mann Linda, Bonten Erik J, d'Azzo Alessandra, Dice J Fred
Department of Anatomy and Structural Biology, Albert Einstein College of Medicine, Bronx, NY 10461, USA.
EMBO J. 2003 Jan 2;22(1):47-59. doi: 10.1093/emboj/cdg002.
Protective protein/cathepsin A (PPCA) has a serine carboxypeptidase activity of unknown physiological function. We now demonstrate that this protease activity triggers the degradation of the lysosome-associated membrane protein type 2a (lamp2a), a receptor for chaperone-mediated autophagy (CMA). Degradation of lamp2a is important because its level in the lysosomal membrane is a rate-limiting step of CMA. Cells defective in PPCA show reduced rates of lamp2a degradation, higher levels of lamp2a and higher rates of CMA. Restoration of PPCA protease activity increases rates of lamp2a degradation, reduces levels of lysosomal lamp2a and reduces rates of CMA. PPCA associates with lamp2a on the lysosomal membrane and cleaves lamp2a near the boundary between the luminal and transmembrane domains. In addition to the well-studied role of PPCA in targeting and protecting two lysosomal glycosidases, we have defined a role for the proteolytic activity of this multifunctional protein.
保护蛋白/组织蛋白酶A(PPCA)具有一种生理功能未知的丝氨酸羧肽酶活性。我们现在证明,这种蛋白酶活性会引发2a型溶酶体相关膜蛋白(lamp2a)的降解,lamp2a是伴侣介导的自噬(CMA)的一种受体。lamp2a的降解很重要,因为其在溶酶体膜中的水平是CMA的一个限速步骤。PPCA缺陷的细胞显示lamp2a降解速率降低、lamp2a水平升高以及CMA速率升高。恢复PPCA蛋白酶活性会增加lamp2a降解速率、降低溶酶体lamp2a水平并降低CMA速率。PPCA与溶酶体膜上的lamp2a结合,并在管腔和跨膜结构域之间的边界附近切割lamp2a。除了PPCA在靶向和保护两种溶酶体糖苷酶方面已得到充分研究的作用外,我们还确定了这种多功能蛋白的蛋白水解活性的作用。