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Gene interactions in cancer

$164,959ZIAFY2022CANIH

Division Of Basic Sciences - Nci

Investigators

Linked publications, trials & patents

Abstract

1. We have contributed to a project in Aldape lab, now published in Acta Neuropathologica Communications. We estimated immune cell type-specific gene expression profiles in 3 large clinically annotated glioma datasets using CIBERSORTx and LM22/LM10 blood-based immune signatures and found that the proportions and estimated gene expression patterns of specific immune cells significantly varied according to IDH mutation status. When IDH-WT and IDH-MUT tumors were considered separately, cluster-of-cluster analyses of immune cell gene expression identified groups with distinct survival outcomes. We then showed a significant association of monocytic lineage cell gene expression clusters with patient survival and with mesenchymal gene expression scores. Integrating immune cell-based gene expression with previously described malignant cell states in glioma demonstrated that macrophage M0 abundance significantly correlated with mesenchymal state in IDH-WT gliomas, with evidence of a previously implicated role of the Oncostatin-M receptor and macrophages in the mesenchymal state. Among IDH-WT tumors that were enriched for the mesenchymal cell state, the estimated M0 macrophage expression signature coordinately also trended to a mesenchymal signature. We also examined IDH-MUT tumors stratified by 1p/19q status, showing that a mesenchymal gene expression signature the M0 macrophage fraction was enriched in IDH-MUT, non-codeleted tumors. Overall, these results highlight the biological and clinical significance of the immune cell environment related to IDH mutation status, patient prognosis and the mesenchymal state in diffuse gliomas. 2. We are now continuing with the above project with goal of specifically identifying functional interactions between specific processes/states across cell types, much like gene-gene interaction approach we have previous published in Cell Reports. 3. A third project we have now initiated with the goal of assessing whether known oncogenic mutations' effect on the clinical phenotype depends on the epigenomic background of the genome. This has implications on precision therapy.

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Gene interactions in cancer · GrantIndex