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与纤溶酶裂解相关的纤维蛋白原和纤维蛋白NH2末端区域的构象和结构调节。

Conformational and structural modulation of the NH2-terminal regions of fibrinogen and fibrin associated with plasmin cleavage.

作者信息

Edgington T S, Plow E F

出版信息

J Biol Chem. 1975 May 10;250(9):3393-8.

PMID:47328
Abstract

Conformational and structural modulations of the NH2-terminal region of fibrinogen and fibrin associated with plasmin cleavage have been examined utilizing specific antibody probes. The E region derived from the NH2-terminal aspects of fibrinogen undergoes complex structural and conformational changes throughout the cleavage process as indicated by differences in the quantitative and qualitative expression of antigenic determinants by the E region of each isolated cleavage fragment. When the range of antigenic determinants recognized by the antibody probe is limited to a specific molecular marker on the gamma chain within the E region, fg-E-neo, evidence for a systematic and progressive modulation of this site during plasmin cleavage is observed. Fg-E-neo undergoes progressive exposure as the cleavage of fibrinogen proceeds from X to Y to D:E complex. Separation of the D:E complex into its constituent, D and E fragments, is associated with further exposure of fg-E-neo determinants. The sequential cleavage of fibrin by plasmin also leads to progressive exposure of the fg-E-neo site; however, comparison of corresponding fragments derived from fibrinogen and fibrin reveals significant differences in the character of fg-E-neo expression. Immunochemical differences between fibrin and fibrinogen E fragments are not abolished by further exposure of the fragments to plasmin, are apparently not due to the presence or absence of fibrinopeptides, and are maintained following denaturation and renaturation of the fragments. These results suggest that the differential expression of fg-E-neo by the E fragments may be primarily dependent upon differences in amino acid compositions of the fragments.

摘要

利用特异性抗体探针,研究了与纤溶酶裂解相关的纤维蛋白原和纤维蛋白氨基末端区域的构象和结构调节。来自纤维蛋白原氨基末端的E区域在整个裂解过程中经历复杂的结构和构象变化,这由每个分离的裂解片段的E区域抗原决定簇的定量和定性表达差异所表明。当抗体探针识别的抗原决定簇范围限于E区域内γ链上的特定分子标记fg-E-neo时,在纤溶酶裂解过程中观察到该位点有系统的、渐进的调节证据。随着纤维蛋白原从X裂解为Y再到D:E复合物,fg-E-neo逐渐暴露。将D:E复合物分离成其组成部分D和E片段,与fg-E-neo决定簇的进一步暴露相关。纤溶酶对纤维蛋白的顺序裂解也导致fg-E-neo位点的逐渐暴露;然而,比较来自纤维蛋白原和纤维蛋白的相应片段发现,fg-E-neo表达的特征存在显著差异。纤维蛋白和纤维蛋白原E片段之间的免疫化学差异不会因片段进一步暴露于纤溶酶而消除,显然不是由于纤维蛋白肽的存在与否,并且在片段变性和复性后仍然存在。这些结果表明,E片段对fg-E-neo的差异表达可能主要取决于片段氨基酸组成的差异。

相似文献

1
Conformational and structural modulation of the NH2-terminal regions of fibrinogen and fibrin associated with plasmin cleavage.与纤溶酶裂解相关的纤维蛋白原和纤维蛋白NH2末端区域的构象和结构调节。
J Biol Chem. 1975 May 10;250(9):3393-8.
2
A cleavage-associated neoantigenic marker for a gamma chain site in the NH2-terminal aspect of the fibrinogen molecule.纤维蛋白原分子氨基末端γ链位点的一种切割相关新抗原标记物。
J Biol Chem. 1975 May 10;250(9):3386-92.
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Discriminating neoantigenic differences between fibrinogen and fibrin derivatives.区分纤维蛋白原和纤维蛋白衍生物之间的新抗原差异。
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The number of D and E regions in the fibrinogen molecule.纤维蛋白原分子中D区和E区的数量。
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Calcium modulates plasmin cleavage of the fibrinogen D fragment gamma chain N-terminus: mapping of monoclonal antibody J88B to a plasmin sensitive domain of the gamma chain.钙调节纤维蛋白原D片段γ链N端的纤溶酶切割:单克隆抗体J88B在γ链纤溶酶敏感结构域的定位。
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Immunochemical mapping of the conformation of human fibrinogen. The gamma 95-264 segment in inaccessible to antibody in native fibrinogen but progressively exposed by plasmic cleavage.人纤维蛋白原构象的免疫化学图谱。γ95 - 264片段在天然纤维蛋白原中无法与抗体结合,但通过血浆裂解逐渐暴露。
J Biol Chem. 1981 Aug 10;256(15):8018-23.

引用本文的文献

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Breakdown products of fibrin and fibrinogen: molecular mechanisms and clinical implications.纤维蛋白和纤维蛋白原的降解产物:分子机制及临床意义
J Clin Pathol Suppl (R Coll Pathol). 1980;14:10-7.
2
Hypotensive activity of histidine-containing analogues of C-terminal hexapeptide of substance P.P物质C末端六肽含组氨酸类似物的降压活性
Experientia. 1986 Apr 15;42(4):417-8. doi: 10.1007/BF02118637.
3
Immune responses to the cleavage-associated neoantigens of fibrinogen in man. Identification and characterization of humoral antibodies specific for cleavage fragments.
人类对纤维蛋白原裂解相关新抗原的免疫反应。对裂解片段特异性体液抗体的鉴定与表征。
J Clin Invest. 1975 Dec;56(6):1509-18. doi: 10.1172/JCI108232.