穆尔-托里综合征相关及散发性皮脂腺肿瘤中MSH-2和MLH-1蛋白表达
MSH-2 and MLH-1 protein expression in Muir Torre syndrome-related and sporadic sebaceous neoplasms.
作者信息
Morales-Burgos Adisbeth, Sánchez Jorge L, Figueroa Luz D, De Jesús-Monge Wilfredo E, Cruz-Correa Marcia R, González-Keelan Carmen, Nazario Cruz María
机构信息
Department of Dermatology, School of Medicine, University of Puerto Rico, San Juan, PR.
出版信息
P R Health Sci J. 2008 Dec;27(4):322-7.
BACKGROUND
Muir-Torre Syndrome (MTS) is a rare autosomal-dominant disorder characterized by the predisposition to both sebaceous neoplasm and internal malignancies. MTS-associated sebaceous neoplasms reveal mutations in DNA mismatch repair (MMR) genes and microsatellite instability. A significant part of MTS patients represents a phenotypic variant, the hereditary nonpolyposis colorectal cancer (HNPCC). A strong correlation between microsatellite instability and immunostaining has been demonstrated. The early recognition of sebaceous neoplasm as part of MTS, and their differentiation from sporadic sebaceous neoplasm may have an important application in a clinical setting. The absence of MLH-1 or MSH-2 expression by immunostaining identifies tumors with mismatch repair deficiency.
OBJECTIVES
Our aim is to determine whether an immunohistochemical approach, targeting DNA repair proteins MSH-2 and MLH-1 in MTS-related sebaceous neoplasm and their sporadic counterparts, can be used for their identification.
METHODS
We examined 15 sebaceous neoplasms (including 6 internal malignancy- associated sebaceous neoplasms and 8 sporadic sebaceous neoplasms) from 11 patients for the expression of MSH-2 and MLH-1 by immunohistochemistry.
RESULTS
Four of 5 internal malignancy-associated sebaceous neoplasms showed loss of expression of MSH-2 or MLH-1. Correlation of the immunostaining pattern of the sebaceous neoplasms and the patients' positive history of colon carcinoma was 80%. Seven of 8 sporadic sebaceous neoplasms showed a positive expression of MSH-2 and MLH-1. The prevalence for loss of expression of MMR proteins in sebaceous neoplasms was 38.5%. MMR immunostaining had 87.5% specificity and 80% sensitivity.
LIMITATIONS
This study is limited by a small sample size, and by bias selection due to the use of non nationwide data-base as the resource of cases.
CONCLUSIONS
Our findings demonstrate that immunohistochemical testing for internal malignancy-associated sebaceous neoplasms is a practical approach to confirm a suspected inherited MMR gene defect, and an accurate method to distinguish between sporadic and MTS-associated sebaceous lesions.
背景
穆尔-托雷综合征(MTS)是一种罕见的常染色体显性疾病,其特征是易患皮脂腺肿瘤和内部恶性肿瘤。与MTS相关的皮脂腺肿瘤显示出DNA错配修复(MMR)基因的突变和微卫星不稳定性。很大一部分MTS患者表现为一种表型变异,即遗传性非息肉病性结直肠癌(HNPCC)。微卫星不稳定性与免疫染色之间已证实存在强相关性。将皮脂腺肿瘤早期识别为MTS的一部分,并将其与散发性皮脂腺肿瘤区分开来,在临床环境中可能具有重要应用价值。免疫染色显示MLH-1或MSH-2表达缺失可识别错配修复缺陷的肿瘤。
目的
我们的目的是确定针对MTS相关皮脂腺肿瘤及其散发性对应肿瘤中的DNA修复蛋白MSH-2和MLH-1的免疫组织化学方法是否可用于它们的识别。
方法
我们通过免疫组织化学检查了11例患者的15个皮脂腺肿瘤(包括6个与内部恶性肿瘤相关的皮脂腺肿瘤和8个散发性皮脂腺肿瘤)中MSH-2和MLH-1的表达情况。
结果
5个与内部恶性肿瘤相关的皮脂腺肿瘤中有4个显示MSH-2或MLH-1表达缺失。皮脂腺肿瘤的免疫染色模式与患者结肠癌阳性病史的相关性为80%。8个散发性皮脂腺肿瘤中有7个显示MSH-2和MLH-1阳性表达。皮脂腺肿瘤中MMR蛋白表达缺失的发生率为38.5%。MMR免疫染色的特异性为87.5%,敏感性为80%。
局限性
本研究受样本量小以及因使用非全国性数据库作为病例来源而导致的偏倚选择的限制。
结论
我们的研究结果表明,对与内部恶性肿瘤相关的皮脂腺肿瘤进行免疫组织化学检测是确认疑似遗传性MMR基因缺陷的实用方法,也是区分散发性和MTS相关皮脂腺病变的准确方法。
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