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Literature DB >> 33708224

PSGL-1 Immune Checkpoint Inhibition for CD4⁺ T Cell Cancer Immunotherapy.

Julia M DeRogatis¹, Karla M Viramontes¹, Emily N Neubert¹, Roberto Tinoco¹.

Abstract

Immune checkpoint inhibition targeting T cells has shown tremendous promise in the treatment of many cancer types and are now standard therapies for patients. While standard therapies have focused on PD-1 and CTLA-4 blockade, additional immune checkpoints have shown promise in promoting anti-tumor immunity. PSGL-1, primarily known for its role in cellular migration, has also been shown to function as a negative regulator of CD4+ T cells in numerous disease settings including cancer. PSGL-1 is highly expressed on T cells and can engage numerous ligands that impact signaling pathways, which may modulate CD4+ T cell differentiation and function. PSGL-1 engagement in the tumor microenvironment may promote CD4+ T cell exhaustion pathways that favor tumor growth. Here we highlight that blocking the PSGL-1 pathway on CD4+ T cells may represent a new cancer therapy approach to eradicate tumors.

Entities: CellLine Chemical Disease Gene Species

Keywords: CD4+ T cells; PSGL-1; anti-tumor immunity; cancer immunology; immune checkpoints

Year: 2021 PMID： 33708224 PMCID： PMC7940186 DOI： 10.3389/fimmu.2021.636238

Source DB: PubMed Journal: Front Immunol ISSN： 1664-3224 Impact factor: 7.561

181 in total

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8. VISTA is a novel broad-spectrum negative checkpoint regulator for cancer immunotherapy.

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2. Targeting the PSGL-1 Immune Checkpoint Promotes Immunity to PD-1-Resistant Melanoma.

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8. PSGL-1 Is a T Cell Intrinsic Inhibitor That Regulates Effector and Memory Differentiation and Responses During Viral Infection.

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