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多内分泌腺瘤2A型家族中突变的直接非放射性检测

Direct, non-radioactive detection of mutations in multiple endocrine neoplasia type 2A families.

作者信息

McMahon R, Mulligan L M, Healey C S, Payne S J, Ponder M, Ferguson-Smith M A, Barton D E, Ponder B A

机构信息

East Anglian Regional Genetics Service, Molecular Genetics Laboratory, Addenbrooke's NHS Trust, Cambridge, UK.

出版信息

Hum Mol Genet. 1994 Apr;3(4):643-6. doi: 10.1093/hmg/3.4.643.

Abstract

We have designed PCR primers that permit the rapid non-isotopic detection of mutations in codon 634 of the RET proto-oncogene, the causative mutations in over 80% of MEN 2A and 50% of FMTC families. In this paper we report the investigation of eleven MEN 2A families referred to the East Anglian Regional Genetics Service. Nine of these families carry codon 634 mutations. We were able to confirm the diagnosis of MEN 2A in twenty six affected individuals and to determine the carrier status of forty one individuals thought to be at risk of developing the disease. Of those at risk, thirty one patients lacked the familial mutation and ten were presymptomatic carriers of MEN 2A. In five cases the direct test proved that patients who had been treated by thyroidectomy but who lacked confirmed cancer, did not carry the familial mutation, removing the perceived risk of MEN 2A from their children. This group included one patient who had been diagnosed as having mild C-cell hyperplasia, confirming that in MEN 2A families C-cell hyperplasia can result from causes other than the presence of the MEN 2A mutation.

摘要

我们设计了聚合酶链反应(PCR)引物,可用于快速非同位素检测RET原癌基因第634密码子的突变,超过80%的2A型多发性内分泌腺瘤(MEN 2A)和50%的家族性甲状腺髓样癌(FMTC)家族的致病突变均源于此。在本文中,我们报告了对转介至东安格利亚地区遗传学服务中心的11个MEN 2A家族的调查情况。其中9个家族携带第634密码子突变。我们得以确诊26名受影响个体的MEN 2A,并确定了41名被认为有患病风险个体的携带者状态。在这些有风险的个体中,31名患者没有家族性突变,10名是MEN 2A的症状前携带者。在5个病例中,直接检测证明,接受过甲状腺切除术但未确诊患有癌症的患者没有家族性突变,从而消除了其子女患MEN 2A的潜在风险。这组患者中有1名曾被诊断为患有轻度C细胞增生,证实了在MEN 2A家族中,C细胞增生可能由MEN 2A突变以外的原因引起。

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