在HeLa细胞中,GGA2的特异性缺失导致组织蛋白酶D的错误分类。

Tatsuhiro Hida, Hiroko Ikeda, Satoshi Kametaka, Chihiro Akazawa, Shinichi Kohsaka, Shigeyuki Ebisu, Yasuo Uchiyama, Satoshi Waguri
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引用次数: 7

摘要

三种哺乳动物GGAs(高尔基定位蛋白、含γ耳蛋白、arf结合蛋白)、GGA1、gg2和gg3参与甘露糖6-磷酸受体(MPR)的分选。为了研究GGA2在溶酶体酶转运中的不同作用,我们建立了两个稳定的细胞系,通过RNA干扰降低了GGA2的表达。GGA2的表达量约为对照水平的5%,而非靶向GGA1和GGA3的表达量未明显降低。GGA2的耗竭并未引起GGA1、GGA3、阳离子依赖型MPR或阳离子依赖型MPR总体分布的变化。此外,GGA2显性负VHS-GAT结构域的适度表达对三种GGAs的反式高尔基网络(TGN)信号没有影响,GGA2信号也不受GGA1或gg3的VHS-GAT结构域表达的影响。这些结果表明,GGA2独立于其他gga被招募到TGN,并且是溶酶体酶的有效分选所必需的。
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Specific depletion of GGA2 causes cathepsin D missorting in HeLa cells.

Three mammalian GGAs (Golgi-localized, gamma-ear-containing, ARF-binding proteins), GGA1, 2, and 3 have been implicated in the sorting of mannose 6-phosphate receptor (MPR). To investigate the distinct roles of GGA2 in lysosomal enzyme transport, we established two stable cell lines that had a reduced expression of GGA2 by RNA interference. The expression levels of GGA2 were approximately 5% of the control levels, whereas those of non-targeted GGA1 and GGA3 were not apparently reduced. The depletion of GGA2 did not cause changes in the overall distribution of GGA1, GGA3, cation-dependent MPR, or cation-independent MPR. However, the cell lines showed increased secretion of a lysosomal enzyme, cathepsin D. In addition, a moderate expression of the dominant negative VHS-GAT domain of GGA2 had no effect on the trans-Golgi network (TGN) signal of three GGAs, nor was the GGA2 signal affected by the expression of VHS-GAT domain of GGA1 or 3. These results suggest that GGA2 is recruited to the TGN independently of the other GGAs and is required for the efficient sorting of lysosomal enzymes.

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来源期刊
Archives of histology and cytology
Archives of histology and cytology 生物-细胞生物学
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期刊介绍: The Archives of Histology and Cytology provides prompt publication in English of original works on the histology and histochemistry of man and animals. The articles published are in principle restricted to studies on vertebrates, but investigations using invertebrates may be accepted when the intention and results present issues of common interest to vertebrate researchers. Pathological studies may also be accepted, if the observations and interpretations are deemed to contribute toward increasing knowledge of the normal features of the cells or tissues concerned. This journal will also publish reviews offering evaluations and critical interpretations of recent studies and theories.
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