Modeling human anti‐pig xenoimmune responses in a pig artery tissue grafted humanized mouse model

Author:

Fang Minghui1,Zou Jun1,Xu Fei1,Wang Xue1,Hua Shucheng2,Zhou Qi34,Yang Yong‐guang15ORCID,Hu Zheng1ORCID

Affiliation:

1. Key Laboratory of Organ Regeneration & Transplantation of Ministry of Education and National‐Local Joint Engineering Laboratory of Animal Models for Human Diseases The First Hospital of Jilin University Changchun China

2. Department of Respiration The First Hospital of Jilin University Changchun China

3. State Key Laboratory of Stem Cell and Reproductive Biology Institute of Zoology Chinese Academy of Sciences Beijing China

4. Institute for Stem Cell and Regeneration Chinese Academy of Sciences Beijing China

5. International Center of Future Science Jilin University Changchun China

Abstract

AbstractBackgroundBlood vessels that contain endothelial cells (ECs) on the surface are in direct contact with host blood and are the first target of xenograft rejection. Currently, our understanding of human anti‐pig vessel immune responses is primarily based on in vitro assays using pig ECs. Therefore, it is necessary to develop an animal model that permits in vivo study of human immunological rejection of pig vessels.MethodsPig artery tissues (PAT) were transplanted into human immune system (HIS) mice or immunodeficient NSG mice (as controls). Intragraft human immune cell infiltration and antibody deposition were quantified using histology and immunohistochemistry. Donor antigen‐specific immune responses were quantified using a mixed lymphocyte reaction and a complement‐dependent killing assay.ResultsPig CD31+ ECs were detected and increased 2‐fold from weeks 3 to 5 in PAT xenografts from immunodeficient NSG mice. However, compared with NSG mice, PAT xenografts in HIS mice had significantly lower numbers of porcine CD31+ ECs and showed a marked reduction from week 3 to week 5. PAT xenograft rejection in HIS mice is associated with intensive infiltration of human immune cells, deposition of human IgM and IgG antibodies, and the formation of a tertiary lymphoid structure. Robust donor pig antigen‐specific human T cells and antibody responses were detected in PAT‐transplanted HIS mice.ConclusionWe have developed a humanized mouse model to evaluate human anti‐pig xenoimmune responses by PAT transplantation in vivo. This model is expected to facilitate the refinement of pig gene‐editing strategies (the expression on EC surface) and the testing of local immunosuppressive strategies for clinical pig organ xenotransplantation.

Funder

National Key Research and Development Program of China

Publisher

Wiley

Subject

Transplantation,Immunology

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