Robust engraftment of fetal nonhuman primate CD34-positive cells in immune-deficient mice

Christopher J Little; William J Haynes; Liupei Huang; Cross M Daffada; Bryce K Wolfe; Elizabeth Perrin; John A Simpson; Jenna A Kropp Schmidt; Hayly M Hinkle; Logan T Keding; Ryan T Behrens; David T Evans; Dixon B Kaufman; James A Thomson; Thaddeus G Golos; Matthew E Brown

doi:10.1002/JLB.5TA0921-481RR

Robust engraftment of fetal nonhuman primate CD34-positive cells in immune-deficient mice

J Leukoc Biol. 2022 Oct;112(4):759-769. doi: 10.1002/JLB.5TA0921-481RR. Epub 2022 Mar 30.

Authors

Christopher J Little¹, William J Haynes¹, Liupei Huang¹, Cross M Daffada¹, Bryce K Wolfe², Elizabeth Perrin³, John A Simpson¹, Jenna A Kropp Schmidt³, Hayly M Hinkle³, Logan T Keding³, Ryan T Behrens⁴, David T Evans^{2

4}, Dixon B Kaufman¹, James A Thomson⁵, Thaddeus G Golos⁶, Matthew E Brown¹

Affiliations

¹ Department of Surgery, Division of Transplantation, University of Wisconsin - Madison, Madison, Wisconsin, USA.
² Department of Pathology and Laboratory Medicine, University of Wisconsin - Madison, Madison, Wisconsin, USA.
³ Wisconsin National Primate Research Center, University of Wisconsin - Madison, Madison, Wisconsin, USA.
⁴ AIDS Vaccine Research Laboratory, University of Wisconsin - Madison, Madison, Wisconsin, USA.
⁵ Morgridge Institute for Research, Madison, Wisconsin, USA.
⁶ Department of Comparative Biosciences, University of Wisconsin - Madison, Madison, Wisconsin, USA.

Abstract

Nonhuman primates (NHPs) represent one of the most important models for preclinical studies of novel biomedical interventions. In contrast with small animal models, however, widespread utilization of NHPs is restricted by cost, logistics, and availability. Therefore, we sought to develop a translational primatized mouse model, akin to a humanized mouse, to allow for high-throughput in vivo experimentation leveraged to inform large animal immunology-based studies. We found that adult rhesus macaque mobilized blood (AMb) CD34+-enriched hematopoietic stem and progenitor cells (HSPCs) engrafted at low but persistent levels in immune-deficient mice harboring transgenes for human (NHP cross-reactive) GM-CSF and IL3, but did not in mice with wild-type murine cytokines lacking NHP cross-reactivity. To enhance engraftment, fetal liver-derived HSPCs were selected as the infusion product based on an increased CD34^hi fraction compared with AMb and bone marrow. Coupled with cotransplantation of rhesus fetal thymic fragments beneath the mouse kidney capsule, fetal liver-derived HSPC infusion in cytokine-transgenic mice yielded robust multilineage lymphohematopoietic engraftment. The emergent immune system recapitulated that of the fetal monkey, with similar relative frequencies of lymphocyte, granulocyte, and monocyte subsets within the thymic, secondary lymphoid, and peripheral compartments. Importantly, while exhibiting a predominantly naïve phenotype, in vitro functional assays demonstrated robust cellular activation in response to nonspecific and allogenic stimuli. This primatized mouse represents a viable and translatable model for the study of hematopoietic stem cell physiology, immune development, and functional immunology in NHPs. Summary Sentence: Engraftment of rhesus macaque hematopoietic tissues in immune-deficient mice yields a robust BLT/NeoThy-type primatized mouse model for studying nonhuman primate hematopoiesis and immune function in vivo.

Keywords: chimerism; hematopoietic stem cells; immune system; primatized mouse; rhesus macaque.

Publication types

Research Support, N.I.H., Extramural

MeSH terms

Animals
Antigens, CD34
Fetal Blood
Granulocyte-Macrophage Colony-Stimulating Factor*
Hematopoietic Stem Cell Transplantation*
Hematopoietic Stem Cells
Humans
Macaca mulatta
Mice
Mice, SCID
Mice, Transgenic

Substances

Antigens, CD34
Granulocyte-Macrophage Colony-Stimulating Factor

Abstract

Publication types

MeSH terms

Substances

Grants and funding