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唾液过氧化物酶(SAPX):基因修饰及其与富含脯氨酸(Pr)蛋白和酸性(Pa)蛋白的关系。

Salivary peroxidase (SAPX): genetic modification and relationship to the proline-rich (Pr) and acidic (Pa) proteins.

作者信息

Azen E A

出版信息

Biochem Genet. 1977 Feb;15(1-2):9-29. doi: 10.1007/BF00484545.

DOI:10.1007/BF00484545
PMID:849256
Abstract

There is genetic polymorphism of the peroxidase of human saliva, but not of leukocytes. The phenotypes are determined by autosomal inheritance, the phenotype of fast mobility (SAPX 1) being determined by homozygosity for a recessive gene (SAPX1) and the phenotypes of slow mobility (SAPX 2 and SAPX 3) being determined by two different genes, SAPX2 and SAPX3, with completely dominant expression at the same locus. The phenotypes are modified by varying degrees of endogenous proteolysis. The SAPX 2 and SAPX 3 types appear to be genetically controlled modifications of SAPX 1 rather than different primary gene products, because of their completely dominant inheritance, their larger molecular size compared to SAPX 1, and their dissociation with 2-mercaptoethanol to give SAPX 1. The acidic protein type Pa 1 is always found in association with SAPX 2, and an uncommon variant type Pa 2 is associated with SAPX 3. The most likely hypothesis is that the genes Pa1 and Pa2 produce products which modify the SAPX 1 type. When the Pa type is Pa 0, the SAPX phenotype is SAPX 1. Since 2-mercaptoethanol can dissociate the Pa 1 protein into a probable monomeric form, and can dissociate SAPX 2 and SAPX 3 to give SAPX 1, it is probable that Pa 1 and Pa 2 monomers complex with SAPX 1 through disulfide bonds to give SAPX 2 or SAPX 3 types. The frequencies of the genes determining the SAPX types are the same as those for Pa: SAPX1 and Pa0 = 0.787, SAPX2 and Pa1 = 0.208, SAPX3 and Pa2 = 0.005.

摘要

人类唾液过氧化物酶存在基因多态性,但白细胞过氧化物酶不存在。其表型由常染色体遗传决定,快速迁移表型(SAPX 1)由隐性基因(SAPX1)的纯合性决定,慢速迁移表型(SAPX 2和SAPX 3)由两个不同基因SAPX2和SAPX3决定,在同一基因座上呈完全显性表达。表型会受到不同程度内源性蛋白水解的影响。SAPX 2和SAPX 3类型似乎是SAPX 1经基因控制的修饰形式,而非不同的初级基因产物,这是因为它们具有完全显性遗传、与SAPX 1相比分子尺寸更大,以及用2-巯基乙醇处理后会解离为SAPX 1。酸性蛋白类型Pa 1总是与SAPX 2相关联,一种罕见的变异类型Pa 2与SAPX 3相关联。最有可能的假说是基因Pa1和Pa2产生的产物会修饰SAPX 1类型。当Pa类型为Pa 0时,SAPX表型为SAPX 1。由于2-巯基乙醇可将Pa 1蛋白解离为可能的单体形式,并可将SAPX 2和SAPX 3解离为SAPX 1,因此很可能Pa 1和Pa 2单体通过二硫键与SAPX 1复合形成SAPX 2或SAPX 3类型。决定SAPX类型的基因频率与Pa的基因频率相同:SAPX1和Pa0 = 0.787,SAPX2和Pa1 = 0.208,SAPX3和Pa2 = 0.005。

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本文引用的文献

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Genetic polymorphism of basic proteins from parotid saliva.腮腺唾液中碱性蛋白的遗传多态性。
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Genetic polymorphism of PIF (parotid isoelectric focusing variant) proteins with linkage to the PPP (parotid proline-rich protein) gene complex.与腮腺富含脯氨酸蛋白(PPP)基因复合体相关的腮腺等电聚焦变异体(PIF)蛋白的遗传多态性。
Biochem Genet. 1981 Jun;19(5-6):475-85. doi: 10.1007/BF00484620.
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Hum Genet. 1985;71(1):30-2. doi: 10.1007/BF00295663.
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Many protein products from a few loci: assignment of human salivary proline-rich proteins to specific loci.少数基因座产生多种蛋白质产物:人类唾液富含脯氨酸蛋白在特定基因座上的定位
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Allelic variants of acidic proline-rich proteins observed in Japanese, Chinese, and Malays.在日本人、中国人和马来人中观察到的富含酸性脯氨酸蛋白的等位基因变体。
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Alleles at the PRB3 locus coding for a disulfide-bonded human salivary proline-rich glycoprotein (Gl 8) and a null in an Ashkenazi Jew.PRB3基因座上的等位基因编码一种二硫键连接的富含脯氨酸的人唾液糖蛋白(Gl 8),在一名阿什肯纳兹犹太人中存在一个无效等位基因。
Am J Hum Genet. 1990 Oct;47(4):686-97.
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Gel electrophoresis: a new catalyst for acid systems.凝胶电泳:酸性体系的新型催化剂。
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5
Size and charge isomer separation and estimation of molecular weights of proteins by disc gel electrophoresis.通过圆盘凝胶电泳进行蛋白质的大小和电荷异构体分离及分子量估计。
Arch Biochem Biophys. 1968 Jul;126(1):155-64. doi: 10.1016/0003-9861(68)90569-9.
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The heterogeneity of human salivary peroxidase.人类唾液过氧化物酶的异质性
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Some properties of the salivary antibacterial factor (S.A.Factor).唾液抗菌因子(S.A.因子)的一些特性。
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Purification and characterization of the salivary antibacterial factor (S.A. factor).唾液抗菌因子(S.A. 因子)的纯化与特性分析
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Polymorphisms of human salivary proteins.人类唾液蛋白的多态性
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Evidence for post-transcriptional modification of human salivary amylase (amyl) isozymes.人类唾液淀粉酶(AMYL)同工酶转录后修饰的证据。
Biochem Genet. 1973 Dec;10(4):341-50. doi: 10.1007/BF00485989.