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. 2025 May 7;17(797):eads2694.
doi: 10.1126/scitranslmed.ads2694. Epub 2025 May 7.

The inhibitory receptor Siglec-E controls antigen-presenting cell activation and T cell-mediated transplant rejection

Thiago J Borges  1 Karina Lima  1 Rodrigo B Gassen  1 Kaifeng Liu  1 Yoshikazu Ganchiku  1 Guilherme T Ribas  1 Minxue Liao  1 Joao I B Goncalves  1 Isadora T Lape  1 Ivy A Rosales  2 Yunlong Zhao  3 Enfu Hui  3 Robert L Fairchild  4   5 Christian LeGuern  1 Cristina Bonorino  6 Stuart K Calderwood  7 Joren C Madsen  1   8 Leonardo V Riella  1   9
Affiliations

The inhibitory receptor Siglec-E controls antigen-presenting cell activation and T cell-mediated transplant rejection

Thiago J Borges et al. Sci Transl Med. .

Abstract

After transplantation, inflammation and tissue injury release danger signals that activate myeloid cells, driving adaptive immune responses and acute rejection. Current immunosuppressants primarily target T cells but inadequately control innate immunity. Regulatory signals controlling innate responses in transplantation remain elusive. The sialic acid-binding immunoglobulin-like lectin-E (Siglec-E, or SigE) binds sialylated ligands to suppress inflammation. In mouse heart transplants, SigE is up-regulated in graft-infiltrating myeloid cells, including dendritic cells (DCs). SigE deficiency in recipients, but not donors, accelerates acute rejection by enhancing DC activation, nuclear factor κB (NF-κB) signaling, and tumor necrosis factor-α (TNF-α) production, thereby boosting alloreactive T cell responses. Conversely, SigE overexpression on DCs reduces activation by danger signals and their T cell allostimulatory capacity. The human homologs Siglecs-7 and -9 were up-regulated in rejecting allograft biopsies, and their higher expression correlated with improved allograft survival. Thus, SigE/7/9 is a crucial inhibitory receptor controlling antigen-presenting cell activation and T cell-mediated transplant rejection, offering therapeutic potential.

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Conflict of interest statement

Competing interests: The authors declare that they have no competing interests.

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