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一种同工酶肿瘤标志物——胎盘碱性磷酸酶的临床及生物学意义

Clinical and biological significance of an isozyme tumor marker--PLAP.

作者信息

Fishman W H

机构信息

La Jolla Cancer Research Foundation, California 92037.

出版信息

Clin Biochem. 1987 Dec;20(6):387-92. doi: 10.1016/0009-9120(87)90003-8.

DOI:10.1016/0009-9120(87)90003-8
PMID:3325192
Abstract

In 1930 the determination of serum alkaline phosphatase in patients with bone or liver disease ushered in the era of clinical enzymology. The association of elevated (bone) alkaline phosphatase in serum of patients with osteogenic sarcoma was the first evidence that tumor cells themselves produced the enzyme. It became clear, however, in the 1960s that the serum alkaline phosphatase was not a single enzyme but consisted of a family of isozymes originating from liver, bone, intestine, and placenta. This was a consequence of the introduction of a combination of electrophoretic separations, heat inactivation, and organ-specific amino acid inhibitors. This combination of measurements made possible the demonstration of a serum alkaline phosphatase of lung cancer origin, as confirmed by the histochemical visualization in lung cancer of the Regan Isozyme (placental alkaline phosphatase-PLAP). At present, the measurement of PLAP has its greatest utility as a tumor marker in seminoma and ovarian cancer. A PLAP-like isozyme in normal testis and ovary is expressed in these and other neoplasias and appears to be related to rare alleles of placental alkaline phosphatase. Current studies have utilized a panel of monoclonal antibodies to detect useful epitopes that suggest that PLAP and PLAP-like isozymes are coded by different genes. The PLAP gene has now been cloned and sequenced by Millan and others. This fundamental new information is providing a base line that will make it possible to explain the overlapping specificities of intestinal and placental isozymes, the degree of uniqueness of the PLAP-like isozyme, the precise mechanism of uncompetitive inhibition by L-phenylalanine and the evolutionary history of the alkaline phosphatases.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

1930年,对骨病或肝病患者血清碱性磷酸酶的测定开创了临床酶学时代。骨肉瘤患者血清中(骨)碱性磷酸酶升高,这是肿瘤细胞自身产生该酶的首个证据。然而,在20世纪60年代,人们清楚地认识到血清碱性磷酸酶并非单一酶,而是由源自肝脏、骨骼、肠道和胎盘的同工酶家族组成。这是采用电泳分离、热灭活和器官特异性氨基酸抑制剂相结合方法的结果。这种测量组合使得能够证实肺癌来源的血清碱性磷酸酶,雷根同工酶(胎盘碱性磷酸酶 - PLAP)在肺癌中的组织化学可视化也证实了这一点。目前,PLAP的测量作为精原细胞瘤和卵巢癌的肿瘤标志物具有最大效用。正常睾丸和卵巢中的一种PLAP样同工酶在这些及其他肿瘤中表达,似乎与胎盘碱性磷酸酶的罕见等位基因有关。当前研究利用一组单克隆抗体来检测有用的表位,这表明PLAP和PLAP样同工酶由不同基因编码。现在Millan等人已克隆并测序了PLAP基因。这一重要的新信息提供了一个基线,将有可能解释肠道和胎盘同工酶的重叠特异性、PLAP样同工酶的独特程度、L - 苯丙氨酸非竞争性抑制的确切机制以及碱性磷酸酶的进化史。(摘要截短于250字)

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