| Literature DB >> 32278152 |
Jiatao Li1, Xisheng Li2, Cai Liang2, Lijun Ling3, Zhiwei Chen3, Chun Kwok Wong2, Herman Waldmann4, Kathy O Lui5.
Abstract
We have previously demonstrated that short-term coreceptor blockade with non-lytic monoclonal antibodies enables the long-term survival of fully allogeneic embryonic stem cell (ESC) transplants in mice. Here, we describe the use of Hu-PBL humanized mice to determine whether short-term coreceptor blockade with humanized anti-human CD4 and CD8 antibodies can achieve the same outcome towards human ESC derivatives. While control Hu-PBL mice rejected allogeneic hESC-derived transplants within weeks, mice treated with coreceptor blocking antibodies held their grafts for 7 weeks, the duration of the study. Rejection in the control mice was associated with demonstrable infiltrates of human CD45 white blood cells, predominantly of CD8 T-cells, whereas anti-CD4, but not anti-CD8 antibody treated mice showed remarkably reduced lymphocyte infiltration and prolonged allograft survival, indicating that the CD4+ T-cells were crucial to the rejection process. Our results give support to the principle that short-term blockade of T-cell co-receptors can achieve long-term acceptance of regenerative cell transplants in humans.Entities:
Keywords: Allograft; Humanized antibodies; Humanized mice; Immunogenicity; Pancreatic beta-like cells; Pluripotent stem cell therapy
Mesh:
Year: 2020 PMID: 32278152 DOI: 10.1016/j.biomaterials.2020.120013
Source DB: PubMed Journal: Biomaterials ISSN: 0142-9612 Impact factor: 12.479