Transcriptional dynamics of colorectal cancer risk associated variation at 11q23.1 are correlated with tuft cell abundance and marker expression <i>in silico</i>-Reference-Cited by-同舟云学术

Transcriptional dynamics of colorectal cancer risk associated variation at 11q23.1 are correlated with tuft cell abundance and marker expression in silico

Published:2022-03-30 Issue: Volume: Page:
ISSN:
Container-title:
language:
Short-container-title:

Author:

Harris Bradley T.^ORCID,Rajasekaran Vidya^ORCID,Blackmur James P.^ORCID,O’Callaghan Alan^ORCID,Donnelly Kevin,Timofeeva Maria^ORCID,Vaughan-Shaw Peter G.^ORCID,Din Farhat V. N.,Dunlop Malcolm G.^ORCID,Farrington Susan M.^ORCID

Abstract

AbstractColorectal cancer (CRC) is characterised by heritable risk that is not well understood. Heritable, genetic variation at 11q23.1 is associated with increased colorectal cancer (CRC) risk, demonstrating eQTL effects on 3 cis- and 23 trans-eQTL targets. We sought to determine the relationship between 11q23.1 cis- and trans-eQTL target expression and test for potential cell-specificity. scRNAseq from 32,361 healthy colonic epithelial cells was aggregated and subject to weighted gene co-expression network analysis (WGCNA). One module (blue) included 19 trans-eQTL targets and was correlated with C11orf53 expression only. Following unsupervised clustering of single cells, the expression of 19 trans-eQTL targets was greatest and most variable in cluster number 11, which transcriptionally resembled tuft cells. 14 trans-eQTL targets were found to demarcate this cluster, 11 of which were corroborated in a second dataset. Intra-cluster WGCNA and module preservation analysis then identified twelve 11q23.1 trans-eQTL targets to comprise a network that was specific to cluster 11. Finally, linear modelling and differential abundance testing showed 11q23.1 trans-eQTL target expression was predictive of cluster 11 abundance. Our findings suggest 11q23.1 trans-eQTL targets comprise a C11orf53-related network that is likely tuft cell-specific and reduced expression of these genes correlates with reduced tuft cell abundance in silico.

Publisher

Cold Spring Harbor Laboratory

Reference49 articles.

1. Banerjee, A. , Herring, C. A. , Chen, B. , Kim, H. , Simmons, A. J. , Southard-Smith, A. N. , Allaman, M. M. , White, J. R. , Macedonia, M. C. , Mckinley, E. T. , Ramirez-Solano, M. A. , Scoville, E. A. , Liu, Q. , Wilson, K. T. , Coffey, R. J. , Washington, M. K. , Goettel, J. A. , & Lau, K. S. (2020). Succinate Produced by Intestinal Microbes Promotes Specification of Tuft Cells to Suppress Ileal Inflammation. Gastroenterology, 159(6). https://doi.org/10.1053/j.gastro.2020.08.029

2. On the Adaptive Control of the False Discovery Rate in Multiple Testing with Independent Statistics

3. Biancolella, M. , Fortini, B. K. , Tring, S. , Plummer, S. J. , Mendoza-Fandino, G. A. , Hartiala, J. , Hitchler, M. J. , Yan, C. , Schumacher, F. R. , Conti, D. v. , Edlund, C. K. , Noushmehr, H. , Coetzee, S. G. , Bresalier, R. S. , Ahnen, D. J. , Barry, E. L. , Berman, B. P. , Rice, J. C. , Coetzee, G. A. , & Casey, G. (2014). Identification and characterization of functional risk variants for colorectal cancer mapping to chromosome 11q23.1. Human Molecular Genetics, 23(8). https://doi.org/10.1093/hmg/ddt584

4. Blackmur, J. P. , Vaughan-Shaw, P. G. , Donnelly, K. , Harris, B. T. , Svinti, V. , Ochocka-Fox, A.-M. , Freile, P. , Walker, M. , Gurran, T. , Reid, S. , Semple, C. A. , Din, F. V. N. , Timofeeva, M. , Dunlop, M. G. , & Farrington, S. M. (2022). Gene Co-Expression Network Analysis Identifies Vitamin D-Associated Gene Modules in Adult Normal Rectal Epithelium Following Supplementation. Frontiers in Genetics, 12. https://doi.org/10.3389/fgene.2021.783970

5. Butts, Carter. T. (2008). network: A package for managing relational data in R. Journal of Statistical Software, 24(2).