首页> 美国卫生研究院文献>The EMBO Journal >Targeting of a lysosomal membrane protein: a tyrosine-containing endocytosis signal in the cytoplasmic tail of lysosomal acid phosphatase is necessary and sufficient for targeting to lysosomes.
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Targeting of a lysosomal membrane protein: a tyrosine-containing endocytosis signal in the cytoplasmic tail of lysosomal acid phosphatase is necessary and sufficient for targeting to lysosomes.

机译:溶酶体膜蛋白的靶向:溶酶体酸性磷酸酶的胞质尾中含酪氨酸的内吞信号对于靶向溶酶体是必要和充分的。

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摘要

Lysosomal acid phosphatase (LAP) is synthesized as a transmembrane protein with a short carboxy-terminal cytoplasmic tail of 19 amino acids, and processed to a soluble protein after transport to lysosomes. Deletion of the membrane spanning domain and the cytoplasmic tail converts LAP to a secretory protein, while deletion of the cytoplasmic tail as well as substitution of tyrosine 413 within the cytoplasmic tail against phenylalanine causes accumulation at the cell surface. A chimeric polypeptide, in which the cytoplasmic tail of LAP was fused to the ectoplasmic and transmembrane domain of hemagglutinin is rapidly internalized and tyrosine 413 of the LAP tail is essential for internalization of the fusion protein. A chimeric polypeptide, in which the membrane spanning domain and cytoplasmic tail of LAP are fused to the ectoplasmic domain of the Mr 46 kd mannose 6-phosphate receptor, is rapidly transported to lysosomes, whereas wild type receptor is not transported to lysosomes. We conclude that a tyrosine containing endocytosis signal in the cytoplasmic tail of LAP is necessary and sufficient for targeting to lysosomes.
机译:溶酶体酸性磷酸酶(LAP)被合成为跨膜蛋白,具有短的19个氨基酸的羧基末端细胞质尾巴,并在转运至溶酶体后加工成可溶性蛋白。跨膜结构域和胞质尾部的缺失将LAP转化为分泌蛋白,而胞质尾部的缺失以及胞质尾部中酪氨酸413对苯丙氨酸的取代导致在细胞表面的积累。嵌合多肽,其中LAP的胞质尾部融合到血凝素的胞质和跨膜结构域,被快速内化,并且LAP尾部的酪氨酸413对于融合蛋白的内化至关重要。嵌合多肽(其中LAP的跨膜结构域和胞质尾部融合到Mr 46 kd甘露糖6-磷酸受体的胞质域上)被快速转运至溶酶体,而野生型受体则未被转运至溶酶体。我们得出结论,在LAP的胞质尾中含有酪氨酸的胞吞信号对于靶向溶酶体是必要和充分的。

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