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在真核生物中搜索 CAML 的远程同源物。

Searching for remote homologs of CAML among eukaryotes.

机构信息

Neuroscience Institute, CNR (Consiglio Nazionale delle Ricerche), Milan, Italy.

出版信息

Traffic. 2020 Oct;21(10):647-658. doi: 10.1111/tra.12758. Epub 2020 Sep 3.

DOI:10.1111/tra.12758
PMID:32715580
Abstract

The tryptophan rich basic protein/calcium signal-modulating cyclophilin ligand (WRB/CAML) and Get1p/Get2p complexes, in vertebrates and yeast, respectively, mediate the final step of tail-anchored protein insertion into the endoplasmic reticulum membrane via the Get pathway. While WRB appears to exist in all eukaryotes, CAML homologs were previously recognized only among chordates, raising the question as to how CAML's function is performed in other phyla. Furthermore, whereas WRB was recognized as the metazoan homolog of Get1, CAML and Get2, although functionally equivalent, were not considered to be homologous. CAML contains an N-terminal basic, TRC40/Get3-interacting, region, three transmembrane segments near the C-terminus, and a poorly conserved region between these domains. Here, I searched the NCBI protein database for remote CAML homologs in all eukaryotes, using position-specific iterated-basic local alignment search tool, with the C-terminal, the N-terminal or the full-length sequence of human CAML as query. The N-terminal basic region and full-length CAML retrieved homologs among metazoa, plants and fungi. In the latter group several hits were annotated as GET2. The C-terminal query did not return entries outside of the animal kingdom, but did retrieve over one hundred invertebrate metazoan CAML-like proteins, which all conserved the N-terminal TRC40-binding domain. The results indicate that CAML homologs exist throughout the eukaryotic domain of life, and suggest that metazoan CAML and yeast GET2 share a common evolutionary origin. They further reveal a tight link between the particular features of the metazoan membrane-anchoring domain and the TRC40-interacting region. The list of sequences presented here should provide a useful resource for future studies addressing structure-function relationships in CAML proteins.

摘要

色氨酸丰富的碱性蛋白/钙信号调节亲环素配体(WRB/CAML)和 Get1p/Get2p 复合物分别在脊椎动物和酵母中介导尾部锚定蛋白插入内质网膜的最后一步,通过 Get 途径。虽然 WRB 似乎存在于所有真核生物中,但 CAML 同源物以前仅在脊索动物中被识别,这就提出了一个问题,即 CAML 的功能在其他门中是如何发挥的。此外,虽然 WRB 被认为是后生动物 Get1 的同源物,但 CAML 和 Get2 虽然功能等效,但不被认为是同源的。CAML 包含一个 N 端碱性、TRC40/Get3 相互作用的区域、靠近 C 端的三个跨膜片段以及这两个结构域之间的保守性较差的区域。在这里,我使用位置特异性迭代基本局部比对搜索工具(position-specific iterated-basic local alignment search tool),以人类 CAML 的 C 端、N 端或全长序列作为查询,在所有真核生物的 NCBI 蛋白质数据库中搜索远程 CAML 同源物。N 端碱性区域和全长 CAML 在后生动物、植物和真菌中检索到同源物。在后一组中,几个命中被注释为 GET2。C 端查询未返回动物王国以外的条目,但检索到一百多种无脊椎后生动物 CAML 样蛋白,它们都保守了 N 端 TRC40 结合结构域。结果表明,CAML 同源物存在于真核生物的生命领域中,并表明后生动物 CAML 和酵母 GET2 具有共同的进化起源。它们进一步揭示了后生动物膜锚定结构域的特定特征与 TRC40 相互作用区域之间的紧密联系。这里呈现的序列列表应该为未来研究 CAML 蛋白的结构-功能关系提供有用的资源。

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1
Searching for remote homologs of CAML among eukaryotes.在真核生物中搜索 CAML 的远程同源物。
Traffic. 2020 Oct;21(10):647-658. doi: 10.1111/tra.12758. Epub 2020 Sep 3.
2
Tail-anchored Protein Insertion in Mammals: FUNCTION AND RECIPROCAL INTERACTIONS OF THE TWO SUBUNITS OF THE TRC40 RECEPTOR.哺乳动物中尾锚定蛋白的插入:TRC40受体两个亚基的功能及相互作用
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WRB and CAML are necessary and sufficient to mediate tail-anchored protein targeting to the ER membrane.WRB和CAML对于介导尾锚定蛋白靶向内质网膜而言是必要且充分的。
PLoS One. 2014 Jan 2;9(1):e85033. doi: 10.1371/journal.pone.0085033. eCollection 2014.
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The Get1/2 transmembrane complex is an endoplasmic-reticulum membrane protein insertase.Get1/2跨膜复合体是一种内质网膜蛋白插入酶。
Nature. 2014 Aug 28;512(7515):441-4. doi: 10.1038/nature13471. Epub 2014 Jul 20.
5
The emerging role of calcium-modulating cyclophilin ligand in posttranslational insertion of tail-anchored proteins into the endoplasmic reticulum membrane.钙调亲环蛋白配体在尾锚定蛋白翻译后插入内质网膜中的新作用。
J Biochem. 2015 Jun;157(6):419-29. doi: 10.1093/jb/mvv035. Epub 2015 Apr 13.
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Endoplasmic reticulum membrane receptors of the GET pathway are conserved throughout eukaryotes.GET 途径的内质网膜受体在真核生物中是保守的。
Proc Natl Acad Sci U S A. 2021 Jan 5;118(1). doi: 10.1073/pnas.2017636118. Epub 2020 Dec 21.
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The WRB Subunit of the Get3 Receptor is Required for the Correct Integration of its Partner CAML into the ER.Get3 受体的 WRB 亚基对于其伴侣 CAML 正确整合到内质网中是必需的。
Sci Rep. 2019 Aug 15;9(1):11887. doi: 10.1038/s41598-019-48363-2.
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The GET complex mediates insertion of tail-anchored proteins into the ER membrane.GET复合体介导尾锚定蛋白插入内质网(ER)膜。
Cell. 2008 Aug 22;134(4):634-45. doi: 10.1016/j.cell.2008.06.025.
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Structural Basis of Tail-Anchored Membrane Protein Biogenesis by the GET Insertase Complex.GET 插入酶复合物介导的尾部锚定膜蛋白生物发生的结构基础。
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10
The mechanism of tail-anchored protein insertion into the ER membrane.尾部锚定蛋白插入内质网膜的机制。
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Endoplasmic reticulum membrane receptors of the GET pathway are conserved throughout eukaryotes.GET 途径的内质网膜受体在真核生物中是保守的。
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