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在肾脏疾病的骨骼肌中表达的心肌肌钙蛋白T同工型不会通过宝灵曼第二代心肌肌钙蛋白T检测法导致假阳性结果。

Cardiac troponin T isoforms expressed in renal diseased skeletal muscle will not cause false-positive results by the second generation cardiac troponin T assay by Boehringer Mannheim.

作者信息

Ricchiuti V, Voss E M, Ney A, Odland M, Anderson P A, Apple F S

机构信息

Department of Laboratory Medicine and Pathology, Hennepin County Medical Center and the University of Minnesota, Minneapolis 55415, USA.

出版信息

Clin Chem. 1998 Sep;44(9):1919-24.

PMID:9732977
Abstract

The purpose of this study was to determine whether the two monoclonal anti-cardiac troponin T (cTnT) antibodies (MAbs) used in the second generation cTnT assay by Boehringer Mannheim (BM, capture Ab, M11.7; detection Ab, M7) would detect cTnT isoforms expressed in human skeletal muscle in response to chronic renal disease (CRD). cTnT expression was examined in skeletal muscle biopsies obtained from 45 CRD patients, as well as nondiseased human heart (n = 3) and skeletal muscle (n = 3). cTnT proteins were resolved by modified 7.5% sodium dodecyl sulfate-polyacrylamide gel electrophoresis, transferred to nitrocellulose, and probed with the following anti-cTnT MAbs: M11.7; M7; JS-2, Lakeland Biomedical; and 13-11, Duke University. All four antibodies detected the cTnT isoforms (Ta, Te) expressed in human myocardium. In 20 of 45 skeletal muscle biopsies, MAb M11.7 recognized its epitope in one to three proteins, molecular mass 34-36 kDa, designated Te, Td, and Tc; the strongest signal was that of Te. The same proteins were recognized by MAbs JS-2 and 13-11. The BM M7 antibody did not detect the cTnT isoforms in the molecular mass range of 34-36 kDa. However, MAb M7 did detect a cTnT isoform, molecular mass 39 kDa, in 2 of 45 biopsies. This isoform had an electrophoretic mobility similar to the predominant heart cTnT isoform, Ta. We conclude that cTnT isoforms are expressed in the skeletal muscle of CRD patients. However, given the epitopes recognized by the BM MAbs M7 and M11.7 and the variable presence of these cTnT isoforms in skeletal muscle, the second generation BM cTnT assay will not detect these isoforms if they are released from skeletal muscle into the circulation.

摘要

本研究的目的是确定勃林格殷格翰公司(BM)第二代心肌肌钙蛋白T(cTnT)检测法中使用的两种单克隆抗心肌肌钙蛋白T抗体(MAb,捕获抗体M11.7;检测抗体M7)是否能检测出慢性肾病(CRD)患者骨骼肌中表达的cTnT同工型。对45例CRD患者的骨骼肌活检样本以及正常人心肌(n = 3)和骨骼肌(n = 3)样本中的cTnT表达情况进行了检测。通过改良的7.5%十二烷基硫酸钠-聚丙烯酰胺凝胶电泳分离cTnT蛋白,转移至硝酸纤维素膜上,并用以下抗cTnT单克隆抗体进行检测:M11.7;M7;JS-2(莱克兰生物医学公司);以及13-11(杜克大学)。所有四种抗体均能检测出人心肌中表达的cTnT同工型(Ta、Te)。在45例骨骼肌活检样本中的20例中,单克隆抗体M11.7在一至三种分子量为34 - 36 kDa的蛋白中识别出其表位,分别命名为Te、Td和Tc;最强信号来自Te。单克隆抗体JS-2和13-11识别出相同的蛋白。BM公司的M7抗体未检测到分子量在34 - 36 kDa范围内的cTnT同工型。然而,单克隆抗体M7在45例活检样本中的2例中检测到一种分子量为39 kDa的cTnT同工型。该同工型的电泳迁移率与主要的心脏cTnT同工型Ta相似。我们得出结论,CRD患者的骨骼肌中表达了cTnT同工型。然而,鉴于BM公司单克隆抗体M7和M11.7识别的表位以及这些cTnT同工型在骨骼肌中的存在情况各异,如果它们从骨骼肌释放到循环系统中,第二代BM cTnT检测法将无法检测到这些同工型。

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