Literature DB >> 20149185

Complement regulation in the GalT KO era.

Shuji Miyagawa1, Aki Yamamoto, Katsuyoshi Matsunami, Dandan Wang, Yuichi Takama, Takehisa Ueno, Masaru Okabe, Hiroshi Nagashima, Masahiro Fukuzawa.   

Abstract

A number of institutes have reported on the successful production of alpha-galactosyltransferase knockout (GalT-KO) pigs. After producing such pigs, hyperacute rejection appeared to no longer be a problem. However, acute vascular rejection (AVR)/acute humoral xenograft rejection (AHXR) is defined as a rejection that begins within 24 h after transplantation and gradually destroys the graft. The origin of AVR/AHXR continues to be a controversial topic, but is generally thought to be initiated by xeno-reactive antibodies, including non-Gal antibodies and subsequent activation of the graft endothelium, the complement and the coagulation systems. The complement is activated via the classical pathway by non-Gal antigens and ischemia-reperfusion injury, via the alternative pathway, especially on islets, and via the lectin pathway. Therefore the complement system is still an important recognition and effector mechanism of AVR/AHXR. In addition, quite recently, based on the relationship between complement and coagulation systems, a new pathway has been proposed. All complement regulatory proteins (CRPs) have the ability to regulate complement activation in different ways. Therefore, to effectively protect xenografts against AVR/AHXR, it appears reasonable to employ not only one but several CRPs including anti-complement drugs. Non-Gal antigens, such as the Hanganutziu-Deicher antigen, is still present on GalT-KO grafts. The further assessment of antigens continues to be an important issue in the area of clinical xenotransplantation. The above conclusions suggest that the expression of human CRPs on GalT-KO grafts is necessary. Moreover, multilateral inhibition of complement activation is required in conjunction with the regulation of the coagulation system.

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Year:  2010        PMID: 20149185     DOI: 10.1111/j.1399-3089.2010.00569.x

Source DB:  PubMed          Journal:  Xenotransplantation        ISSN: 0908-665X            Impact factor:   3.907


  18 in total

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Journal:  Xenotransplantation       Date:  2011 Mar-Apr       Impact factor: 3.907

2.  Trial using pig cells with the H-D antigen knocked down.

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3.  Generation by somatic cell nuclear transfer of GGTA1 knockout pigs expressing soluble human TNFRI-Fc and human HO-1.

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Journal:  Transgenic Res       Date:  2018-12-14       Impact factor: 2.788

Review 4.  The complex functioning of the complement system in xenotransplantation.

Authors:  Hongmin Zhou; Hidetaka Hara; David K C Cooper
Journal:  Xenotransplantation       Date:  2019-04-29       Impact factor: 3.907

Review 5.  Clinical lung xenotransplantation--what donor genetic modifications may be necessary?

Authors:  David K C Cooper; Burcin Ekser; Christopher Burlak; Mohamed Ezzelarab; Hidetaka Hara; Leela Paris; A Joseph Tector; Carol Phelps; Agnes M Azimzadeh; David Ayares; Simon C Robson; Richard N Pierson
Journal:  Xenotransplantation       Date:  2012 May-Jun       Impact factor: 3.907

6.  Lectin array analysis for wild-type and α-Gal-knockout pig islets versus healthy human islets.

Authors:  Shuji Miyagawa; Akira Maeda; Shunsaku Takeishi; Takehisa Ueno; Noriaki Usui; Shinichi Matsumoto; Teru Okitsu; Masafumi Goto; Hiroshi Nagashima
Journal:  Surg Today       Date:  2013-04-03       Impact factor: 2.549

Review 7.  Therapeutic issues in the treatment of vascularized xenotransplants using gal-knockout donors in nonhuman primates.

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Review 8.  Lung xenotransplantation: a review.

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9.  Dual islet transplantation modeling of the instant blood-mediated inflammatory reaction.

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Journal:  Am J Transplant       Date:  2015-02-19       Impact factor: 8.086

10.  Characterization of immunogenic Neu5Gc in bioprosthetic heart valves.

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Journal:  Xenotransplantation       Date:  2016-09-09       Impact factor: 3.907

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