Transcriptome-wide Mendelian randomization during CD4+ T cell activation reveals immune-related drug targets for cardiometabolic diseases

Xueyan Wu; Hui Ying; Qianqian Yang; Qian Yang; Haoyu Liu; Yilan Ding; Huiling Zhao; Zhihe Chen; Ruizhi Zheng; Hong Lin; Shuangyuan Wang; Mian Li; Tiange Wang; Zhiyun Zhao; Min Xu; Yuhong  Chen; Yu Xu; Emma E Vincent; Maria C Borges; Tom R Gaunt; Guang Ning; Weiqing Wang; Yufang Bi; Jie Zheng; Jieli Lu

doi:10.1038/s41467-024-53621-7

Transcriptome-wide Mendelian randomization during CD4+ T cell activation reveals immune-related drug targets for cardiometabolic diseases

Xueyan Wu, Hui Ying, Qianqian Yang, Qian Yang, Haoyu Liu, Yilan Ding, Huiling Zhao, Zhihe Chen, Ruizhi Zheng, Hong Lin, Shuangyuan Wang, Mian Li, Tiange Wang, Zhiyun Zhao, Min Xu, Yuhong Chen, Yu Xu, Emma E Vincent, Maria C Borges, Tom R GauntGuang Ning, Weiqing Wang^*, Yufang Bi^*, Jie Zheng^*, Jieli Lu^*

^*Corresponding author for this work

Research output: Contribution to journal › Article (Academic Journal) › peer-review

12 Citations (Scopus)

Abstract

Immunity has shown potentials in informing drug development for cardiometabolic diseases, such as type 2 diabetes (T2D) and coronary artery disease (CAD). Here, we performed a transcriptome-wide Mendelian randomization (MR) study to estimate the putative causal effects of 11,021 gene expression profiles during CD4+ T cells activation on the development of T2D and CAD. Robust MR and colocalization evidence was observed for 162 genes altering T2D risk and 80 genes altering CAD risk, with 12% and 16% respectively demonstrating CD4+ T cell specificity. We observed temporal causal patterns during T cell activation in 69 gene-T2D pairs and 34 gene-CAD pairs. These genes were eight times more likely to show robust genetic evidence. We further identified 25 genes that were targets for drugs under clinical investigation, including LIPA and GCK. This study provides evidence to support immune-to-metabolic disease connections, and prioritises immune-mediated drug targets for cardiometabolic diseases.

Original language	English
Article number	9302
Number of pages	16
Journal	Nature Communications
Volume	15
DOIs	https://doi.org/10.1038/s41467-024-53621-7
Publication status	Published - 28 Oct 2024

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8074 (C18281/A29019) ICEP2 - Programme Award: Towards improved casual evidence and enhanced prediction of cancer risk and survival
Martin, R. M. (Principal Investigator)
1/10/20 → 30/09/25
Project: Research

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Wu, X., Ying, H., Yang, Q., Yang, Q., Liu, H., Ding, Y., Zhao, H., Chen, Z., Zheng, R., Lin, H., Wang, S., Li, M., Wang, T., Zhao, Z., Xu, M., Chen, Y., Xu, Y., Vincent, E. E., Borges, M. C., ... Lu, J. (2024). Transcriptome-wide Mendelian randomization during CD4+ T cell activation reveals immune-related drug targets for cardiometabolic diseases. Nature Communications, 15, Article 9302. https://doi.org/10.1038/s41467-024-53621-7

@article{2341d4dd095b42a7a43f37b8bbe9414d,

title = "Transcriptome-wide Mendelian randomization during CD4+ T cell activation reveals immune-related drug targets for cardiometabolic diseases",

abstract = "Immunity has shown potentials in informing drug development for cardiometabolic diseases, such as type 2 diabetes (T2D) and coronary artery disease (CAD). Here, we performed a transcriptome-wide Mendelian randomization (MR) study to estimate the putative causal effects of 11,021 gene expression profiles during CD4+ T cells activation on the development of T2D and CAD. Robust MR and colocalization evidence was observed for 162 genes altering T2D risk and 80 genes altering CAD risk, with 12\% and 16\% respectively demonstrating CD4+ T cell specificity. We observed temporal causal patterns during T cell activation in 69 gene-T2D pairs and 34 gene-CAD pairs. These genes were eight times more likely to show robust genetic evidence. We further identified 25 genes that were targets for drugs under clinical investigation, including LIPA and GCK. This study provides evidence to support immune-to-metabolic disease connections, and prioritises immune-mediated drug targets for cardiometabolic diseases.",

author = "Xueyan Wu and Hui Ying and Qianqian Yang and Qian Yang and Haoyu Liu and Yilan Ding and Huiling Zhao and Zhihe Chen and Ruizhi Zheng and Hong Lin and Shuangyuan Wang and Mian Li and Tiange Wang and Zhiyun Zhao and Min Xu and Yuhong Chen and Yu Xu and Vincent, \{Emma E\} and Borges, \{Maria C\} and Gaunt, \{Tom R\} and Guang Ning and Weiqing Wang and Yufang Bi and Jie Zheng and Jieli Lu",

year = "2024",

month = oct,

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doi = "10.1038/s41467-024-53621-7",

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Wu, X, Ying, H, Yang, Q, Yang, Q, Liu, H, Ding, Y, Zhao, H, Chen, Z, Zheng, R, Lin, H, Wang, S, Li, M, Wang, T, Zhao, Z, Xu, M, Chen, Y, Xu, Y, Vincent, EE , Borges, MC , Gaunt, TR, Ning, G, Wang, W, Bi, Y, Zheng, J & Lu, J 2024, 'Transcriptome-wide Mendelian randomization during CD4+ T cell activation reveals immune-related drug targets for cardiometabolic diseases', Nature Communications, vol. 15, 9302. https://doi.org/10.1038/s41467-024-53621-7

TY - JOUR

T1 - Transcriptome-wide Mendelian randomization during CD4+ T cell activation reveals immune-related drug targets for cardiometabolic diseases

AU - Wu, Xueyan

AU - Ying, Hui

AU - Yang, Qianqian

AU - Yang, Qian

AU - Liu, Haoyu

AU - Ding, Yilan

AU - Zhao, Huiling

AU - Chen, Zhihe

AU - Zheng, Ruizhi

AU - Lin, Hong

AU - Wang, Shuangyuan

AU - Li, Mian

AU - Wang, Tiange

AU - Zhao, Zhiyun

AU - Xu, Min

AU - Chen, Yuhong

AU - Xu, Yu

AU - Vincent, Emma E

AU - Borges, Maria C

AU - Gaunt, Tom R

AU - Ning, Guang

AU - Wang, Weiqing

AU - Bi, Yufang

AU - Zheng, Jie

AU - Lu, Jieli

PY - 2024/10/28

Y1 - 2024/10/28

N2 - Immunity has shown potentials in informing drug development for cardiometabolic diseases, such as type 2 diabetes (T2D) and coronary artery disease (CAD). Here, we performed a transcriptome-wide Mendelian randomization (MR) study to estimate the putative causal effects of 11,021 gene expression profiles during CD4+ T cells activation on the development of T2D and CAD. Robust MR and colocalization evidence was observed for 162 genes altering T2D risk and 80 genes altering CAD risk, with 12% and 16% respectively demonstrating CD4+ T cell specificity. We observed temporal causal patterns during T cell activation in 69 gene-T2D pairs and 34 gene-CAD pairs. These genes were eight times more likely to show robust genetic evidence. We further identified 25 genes that were targets for drugs under clinical investigation, including LIPA and GCK. This study provides evidence to support immune-to-metabolic disease connections, and prioritises immune-mediated drug targets for cardiometabolic diseases.

AB - Immunity has shown potentials in informing drug development for cardiometabolic diseases, such as type 2 diabetes (T2D) and coronary artery disease (CAD). Here, we performed a transcriptome-wide Mendelian randomization (MR) study to estimate the putative causal effects of 11,021 gene expression profiles during CD4+ T cells activation on the development of T2D and CAD. Robust MR and colocalization evidence was observed for 162 genes altering T2D risk and 80 genes altering CAD risk, with 12% and 16% respectively demonstrating CD4+ T cell specificity. We observed temporal causal patterns during T cell activation in 69 gene-T2D pairs and 34 gene-CAD pairs. These genes were eight times more likely to show robust genetic evidence. We further identified 25 genes that were targets for drugs under clinical investigation, including LIPA and GCK. This study provides evidence to support immune-to-metabolic disease connections, and prioritises immune-mediated drug targets for cardiometabolic diseases.

U2 - 10.1038/s41467-024-53621-7

DO - 10.1038/s41467-024-53621-7

M3 - Article (Academic Journal)

C2 - 39468075

SN - 2041-1723

VL - 15

JO - Nature Communications

JF - Nature Communications

M1 - 9302

ER -

Transcriptome-wide Mendelian randomization during CD4+ T cell activation reveals immune-related drug targets for cardiometabolic diseases

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8074 (C18281/A29019) ICEP2 - Programme Award: Towards improved casual evidence and enhanced prediction of cancer risk and survival

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