Engagement of sialylated glycans with Siglec receptors on suppressive myeloid cells inhibits anticancer immunity via CCL2.
Ronja WieboldtMichael SandholzerEmanuele CarliniChia-Wei LinAnastasiya BörschAndreas ZinggDidier LardinoisPetra HerzigLeyla DonAlfred ZippeliusHeinz LaubliNatalia Rodrigues MantuanoPublished in: Cellular & molecular immunology (2024)
The overexpression of sialic acids on glycans, called hypersialylation, is a common alteration found in cancer cells. Sialylated glycans can enhance immune evasion by interacting with sialic acid-binding immunoglobulin-like lectin (Siglec) receptors on tumor-infiltrating immune cells. Here, we investigated the effect of sialylated glycans and their interaction with Siglec receptors on myeloid-derived suppressor cells (MDSCs). We found that MDSCs derived from the blood of lung cancer patients and tumor-bearing mice strongly express inhibitory Siglec receptors and are highly sialylated. In murine cancer models of emergency myelopoiesis, Siglec-E knockout in myeloid cells resulted in prolonged survival and increased tumor infiltration of activated T cells. Targeting suppressive myeloid cells by blocking Siglec receptors or desialylation strongly reduced their suppressive potential. We further identified CCL2 as a mediator involved in T-cell suppression upon interaction between sialoglycans and Siglec receptors on MDSCs. Our results demonstrated that sialylated glycans inhibit anticancer immunity by modulating CCL2 expression.
Keyphrases
- liver fibrosis
- induced apoptosis
- cell cycle arrest
- cell surface
- emergency department
- dendritic cells
- acute myeloid leukemia
- bone marrow
- public health
- cell death
- signaling pathway
- type diabetes
- healthcare
- poor prognosis
- squamous cell carcinoma
- cell proliferation
- social media
- metabolic syndrome
- young adults
- skeletal muscle
- drug delivery
- cancer therapy
- risk assessment
- childhood cancer