Abstract: Immunological memory specific to previously encountered antigens is a cardinal feature of adaptive lymphoid cells.  It is not known however whether innate myeloid cells retain memory of prior antigenic stimulation and respond to it more vigorously upon a second encounter.  Here, we show that murine monocytes and macrophages acquire memory specific to MHC-I antigens and identify paired immunoglobulin-like receptors-A (PIR-A) as the MHC-I receptors necessary for the memory response.  We demonstrate that deleting PIR-A in the recipient or blocking PIR-A binding to donor MHC-I molecules blocks memory and attenuates kidney and heart allograft rejection.  Thus, innate myeloid cells acquire alloantigen-specific memory that can be targeted to improve transplant outcomes.;	Data purpose: Targeting monocyte and macrophage receptors that detect MHC antigens blocks innate immune memory and attenuates transplant rejection SOURCE: Wei Chen (wei.chen@chp.edu) -  Children’s Hospital of Pittsburgh of UPMC

Pluto Bioinformatics

GSE147596: Paired immunoglobulin-like receptors mediate innate memory to non-self MHC molecules