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猪因子VII、X的特性及其与人类因子VII、X的比较

Characterization of porcine factor VII, X and comparison with human factor VII, X.

作者信息

Chen Younan, Qiao Jianlin, Tan Weidong, Lu Yanrong, Qin Shengfang, Zhang Jie, Li Shengfu, Bu Hong, Cheng Jingqiu

机构信息

Key Laboratory of Transplant Engineering and Immunology, Ministry of Health, West China Hospital, Sichuan University, PR China.

出版信息

Blood Cells Mol Dis. 2009 Jul-Aug;43(1):111-8. doi: 10.1016/j.bcmd.2009.02.004. Epub 2009 Mar 16.

Abstract

OBJECTIVE

Factor VII (FVII) and factor X (FX) are two predominant molecules of coagulation cascade. Whether porcine FVII and FX could efficiently work in human circulation is important for successful pig to human liver transplantation. We compared the genetic characterizations and coagulation activities of porcine and human FVII and FX to shed insight into the further investigation of potential inter-species molecular incompatibility between porcine FVII, FX and human derived procoagulants and anticoagulants in xenotransplantation.

METHODS

Multiple rounds of PCR were used to screen the positive clones from a porcine liver tissue cDNA library. 5' RACE and 3' RACE were conducted to get the full-length cDNA. The three-dimensional structure of protein was modeled by Swiss-Model program. Prothrombin Time (PT) of porcine and human plasma was determined by coagulation autoanalyzer. Activities of porcine FVII and FX were detected by adding the porcine plasma into FVII or FX-deficient human plasma.

RESULTS

We cloned the full-length cDNA of porcine FVII and FX, which contained 1416 bp and 1856 bp, coding 445 and 479 amino acids, respectively. Porcine FVII and FX shared 74.08% and 73.1% amino acid identities with human FVII and FX. Sequence alignments showed that porcine FVII might have additional gamma-carboxyglutamic acid in Gla domain, and one important variation of Lys62-Glu in light chain. No significant difference was observed in TF binding region of heavy chain, while 4 variations were identified in the important functional residues responsible for proteolysis activity, as Gln217-Glu, Thr151-Lys, Glu154-Val and Gln40-Leu. However, no apparent change was displayed in the 3-D model of the heavy chain of porcine FVII. When porcine FX was analyzed, great variations have been found at active peptide (Ser143 to Arg194) with only 11.6% identity. Some important variations at gamma-carboxyglutamic acids and Ca(2+) binding sites were identified, while high conservations were discovered at other functional sites. Comparisons on 3-D protein models demonstrated that the protein backbones of porcine and human FX were highly conserved, and little difference was shown at the molecular surface of anticoagulant binding sites S2 and S3. PT detection of porcine and human plasma showed similar results, while coagulation activities of porcine FVII and FX were remarkably higher than that of human.

CONCLUSION

Porcine FVII and FX showed relatively high homology with human FVII and FX in nucleotide, amino acid sequences and three-dimensional structure. However, the different affinities to important macromolecules caused by genetic differences might contribute to the molecular incompatibilities in liver xenotransplantation.

摘要

目的

凝血因子VII(FVII)和凝血因子X(FX)是凝血级联反应中的两个主要分子。猪的FVII和FX能否在人体循环中有效发挥作用对于猪到人的肝脏移植成功至关重要。我们比较了猪和人FVII及FX的遗传特征和凝血活性,以深入了解异种移植中猪FVII、FX与人类来源的促凝血剂和抗凝剂之间潜在的种间分子不相容性的进一步研究。

方法

通过多轮PCR从猪肝组织cDNA文库中筛选阳性克隆。进行5' RACE和3' RACE以获得全长cDNA。利用Swiss - Model程序对蛋白质的三维结构进行建模。用凝血自动分析仪测定猪和人血浆的凝血酶原时间(PT)。通过将猪血浆加入FVII或FX缺乏的人血浆中来检测猪FVII和FX的活性。

结果

我们克隆了猪FVII和FX的全长cDNA,分别包含1416 bp和1856 bp,分别编码445和479个氨基酸。猪FVII和FX与人FVII和FX的氨基酸同源性分别为74.08%和73.1%。序列比对显示猪FVII在Gla结构域可能有额外的γ-羧基谷氨酸,并且轻链中有一个重要的Lys62 - Glu变异。重链的TF结合区域未观察到显著差异,而在负责蛋白水解活性的重要功能残基中鉴定出4个变异,即Gln217 - Glu、Thr151 - Lys、Glu154 - Val和Gln40 - Leu。然而,猪FVII重链的三维模型中未显示明显变化。分析猪FX时,在活性肽(Ser143至Arg194)处发现了很大差异,同源性仅为11.6%。在γ-羧基谷氨酸和Ca(2+)结合位点鉴定出一些重要变异,而在其他功能位点发现高度保守性。对蛋白质三维模型的比较表明,猪和人FX的蛋白质主链高度保守,在抗凝剂结合位点S2和S3的分子表面显示出微小差异。猪和人血浆的PT检测结果相似,而猪FVII和FX的凝血活性明显高于人。

结论

猪FVII和FX在核苷酸、氨基酸序列及三维结构上与人FVII和FX显示出相对较高的同源性。然而,由遗传差异导致的对重要大分子的不同亲和力可能导致肝脏异种移植中的分子不相容性。

相似文献

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Characterization of porcine factor VII, X and comparison with human factor VII, X.猪因子VII、X的特性及其与人类因子VII、X的比较
Blood Cells Mol Dis. 2009 Jul-Aug;43(1):111-8. doi: 10.1016/j.bcmd.2009.02.004. Epub 2009 Mar 16.

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