Pig Thrombomodulin Binds Human Thrombin but is a Poor Cofactor for Activation of Human Protein C and TAFI

Overview

Journal Am J Transplant

Publisher Elsevier

Specialty General Surgery

Date 2008 May 1

PMID 18444940

Citations 47

Authors

J C Roussel

C J Moran

E J Salvaris

H H Nandurkar

A J F dApice

P J Cowan

Affiliations

Soon will be listed here.

Abstract

Incompatibility between pig thrombomodulin (TM) and primate thrombin is thought to be an important factor in the development of microvascular thrombosis in rejecting pig-to-primate xenografts. To examine this interaction at the molecular level, we cloned pig TM and measured its ability to bind human thrombin and act as a cofactor for the activation of human protein C and TAFI. The 579-residue pig TM protein showed approximately 69% sequence identity to human TM. Within the EGF domains necessary for binding of thrombin (EGF56), protein C (EGF4) and TAFI (EGF3), all of the amino acids previously identified as critical for the function of human TM, with the exception of Glu-408 in EGF5, were conserved in pig TM. Comparison of transfected cells expressing pig or human TM demonstrated that both proteins bound human thrombin and inhibited its procoagulant activity. However, pig TM was a poor cofactor for the activation of human protein C and TAFI, with domain swapping showing that EGF5 was the most important determinant of compatibility. Thus, while pig TM may be capable of binding thrombin generated in the vicinity of xenograft endothelium, its failure to promote the activation of human protein C remains a significant problem.

Citing Articles

Systematic Review and Comparative Outcomes Analysis of NHP Liver Allotransplants and Xenotransplants.

Shirini K, Meier R Xenotransplantation. 2025; 32(1):e70017.

PMID: 39960351 PMC: 11832012. DOI: 10.1111/xen.70017.

Immunometabolism of Liver Xenotransplantation and Prospective Solutions.

Deng S, Zhang Y, Shen S, Li C, Qin C Adv Sci (Weinh). 2025; 12(9):e2407610.

PMID: 39912334 PMC: 11884532. DOI: 10.1002/advs.202407610.

The generation and evaluation of TKO/hCD55/hTM/hEPCR gene-modified pigs for clinical organ xenotransplantation.

Huai G, Wang Y, Du J, Cheng Z, Xie Y, Zhou J Front Immunol. 2025; 15:1488552.

PMID: 39902050 PMC: 11788277. DOI: 10.3389/fimmu.2024.1488552.

Characterizing coagulation responses in humans and nonhuman primates following kidney xenotransplantation-A narrative review.

Zidan A, El-Sherbini A, Noureldin A, Cooper D, Othman M Am J Hematol. 2024; 100(2):285-295.

PMID: 39404060 PMC: 11705208. DOI: 10.1002/ajh.27506.

Cutting edge of immune response and immunosuppressants in allogeneic and xenogeneic islet transplantation.

Yue L, Li J, Yao M, Song S, Zhang X, Wang Y Front Immunol. 2024; 15:1455691.

PMID: 39346923 PMC: 11427288. DOI: 10.3389/fimmu.2024.1455691.