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人羧肽酶 A6 的底物特异性。

Substrate specificity of human carboxypeptidase A6.

机构信息

Department of Molecular Pharmacology, Albert Einstein College of Medicine, Bronx, New York 10461, USA.

出版信息

J Biol Chem. 2010 Dec 3;285(49):38234-42. doi: 10.1074/jbc.M110.158626. Epub 2010 Sep 20.

Abstract

Carboxypeptidase A6 (CPA6) is an extracellular matrix-bound metallocarboxypeptidase (CP) that has been implicated in Duane syndrome, a neurodevelopmental disorder in which the lateral rectus extraocular muscle is not properly innervated. Consistent with a role in Duane syndrome, CPA6 is expressed in a number of chondrocytic and nervous tissues during embryogenesis. To better characterize the enzymatic function and specificity of CPA6 and to compare this with other CPs, CPA6 was expressed in HEK293 cells and purified. Kinetic parameters were determined using a panel of synthetic carboxypeptidase substrates, indicating a preference of CPA6 for large hydrophobic C-terminal amino acids and only very weak activity toward small amino acids and histidine. A quantitative peptidomics approach using a mixture of peptides representative of the neuropeptidome allowed the characterization of CPA6 preferences at the P1 substrate position and suggested that small and acidic P1 residues significantly inhibit CPA6 cleavage. Finally, a comparison of available kinetic data for CPA enzymes shows a gradient of specificity across the subfamily, from the very restricted specificity of CPA2 to the very broad activity of CPA4. Structural data and modeling for all CPA/B subfamily members suggests the structural basis for the unique specificities observed for each member of the CPA/B subfamily of metallocarboxypeptidases.

摘要

羧肽酶 A6(CPA6)是一种细胞外基质结合的金属羧肽酶(CP),与神经发育障碍性疾病杜安综合征有关,在这种疾病中,外直肌的神经支配不正常。与杜安综合征的作用一致,CPA6 在胚胎发生过程中在许多软骨细胞和神经组织中表达。为了更好地描述 CPA6 的酶学功能和特异性,并与其他 CP 进行比较,我们在 HEK293 细胞中表达和纯化了 CPA6。使用一系列合成羧肽酶底物测定了动力学参数,表明 CPA6 优先选择大的疏水性 C 末端氨基酸,对小氨基酸和组氨酸的活性非常弱。使用混合肽代表神经肽组的定量肽组学方法,可表征 CPA6 在 P1 底物位置的偏好性,并表明小的和酸性的 P1 残基显著抑制 CPA6 的切割。最后,对可用的 CPA 酶动力学数据进行比较,显示出整个亚家族的特异性梯度,从 CPA2 的非常受限的特异性到 CPA4 的非常广泛的活性。所有 CPA/B 亚家族成员的结构数据和建模表明了金属羧肽酶 CPA/B 亚家族每个成员所观察到的独特特异性的结构基础。

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