Systematic in vivo candidate evaluation uncovers therapeutic targets for LMNA dilated cardiomyopathy and risk of Lamin A toxicity

Chia Yee Tan; Pui Shi Chan; Hansen Tan; Sung Wei Tan; Chang Jie Mick Lee; Jiong-Wei Wang; Shu Ye; Hendrikje Werner; Ying Jie Loh; Yin Loon Lee; Matthew Ackers-Johnson; Roger S Y Foo; Jianming Jiang

doi:10.1186/s12967-023-04542-4

Systematic in vivo candidate evaluation uncovers therapeutic targets for LMNA dilated cardiomyopathy and risk of Lamin A toxicity

J Transl Med. 2023 Oct 16;21(1):690. doi: 10.1186/s12967-023-04542-4.

Authors

Chia Yee Tan^{1

2

3}, Pui Shi Chan^{1

2

3}, Hansen Tan^{1

2

3}, Sung Wei Tan^{1

2

3}, Chang Jie Mick Lee^{2

3}, Jiong-Wei Wang^{2

4

5

6}, Shu Ye^{2

3}, Hendrikje Werner⁷, Ying Jie Loh⁷, Yin Loon Lee^{7

8}, Matthew Ackers-Johnson^{2

3}, Roger S Y Foo^{2

3}, Jianming Jiang^{9

10

11}

Affiliations

¹ Department of Biochemistry, Yong Loo Lin School of Medicine, National University of Singapore, Singapore, 117597, Singapore.
² Centre for Translational Medicine, Cardiovascular Research Institute (CVRI), National University Health System, 14 Medical Drive, Singapore, 117599, Singapore.
³ Cardiovascular Disease Translational Research Programme, NUS Yong Loo Lin School of Medicine, 14 Medical Drive, Level 8, Singapore, 117599, Singapore.
⁴ Department of Surgery, Yong Loo Lin School of Medicine, National University of Singapore, Singapore, 119228, Singapore.
⁵ Centre for NanoMedicine, Nanomedicine Translational Research Programme, Yong Loo Lin School of Medicine, National University of Singapore, Singapore, 117609, Singapore.
⁶ Department of Physiology, National University of Singapore, Singapore, 117593, Singapore.
⁷ Nuevocor Pte Ltd, 1 Biopolis Drive, Amnios, #05-01, Singapore, 138622, Singapore.
⁸ A*STAR Skin Research Labs (A*SRL), Agency for Science, Technology and Research (A*STAR), 8A Biomedical Grove, Immunos #06-06, Singapore, 138665, Singapore.
⁹ Department of Biochemistry, Yong Loo Lin School of Medicine, National University of Singapore, Singapore, 117597, Singapore. bchjian@nus.edu.sg.
¹⁰ Centre for Translational Medicine, Cardiovascular Research Institute (CVRI), National University Health System, 14 Medical Drive, Singapore, 117599, Singapore. bchjian@nus.edu.sg.
¹¹ Cardiovascular Disease Translational Research Programme, NUS Yong Loo Lin School of Medicine, 14 Medical Drive, Level 8, Singapore, 117599, Singapore. bchjian@nus.edu.sg.

Abstract

Background: Dilated cardiomyopathy (DCM) is a severe, non-ischemic heart disease which ultimately results in heart failure (HF). Decades of research on DCM have revealed diverse aetiologies. Among them, familial DCM is the major form of DCM, with pathogenic variants in LMNA being the second most common form of autosomal dominant DCM. LMNA DCM is a multifactorial and complex disease with no specific treatment thus far. Many studies have demonstrated that perturbing candidates related to various dysregulated pathways ameliorate LMNA DCM. However, it is unknown whether these candidates could serve as potential therapeutic targets especially in long term efficacy.

Methods: We evaluated 14 potential candidates including Lmna gene products (Lamin A and Lamin C), key signaling pathways (Tgfβ/Smad, mTor and Fgf/Mapk), calcium handling, proliferation regulators and modifiers of LINC complex function in a cardiac specific Lmna DCM model. Positive candidates for improved cardiac function were further assessed by survival analysis. Suppressive roles and mechanisms of these candidates in ameliorating Lmna DCM were dissected by comparing marker gene expression, Tgfβ signaling pathway activation, fibrosis, inflammation, proliferation and DNA damage. Furthermore, transcriptome profiling compared the differences between Lamin A and Lamin C treatment.

Results: Cardiac function was restored by several positive candidates (Smad3, Yy1, Bmp7, Ctgf, aYAP1, Sun1, Lamin A, and Lamin C), which significantly correlated with suppression of HF/fibrosis marker expression and cardiac fibrosis in Lmna DCM. Lamin C or Sun1 shRNA administration achieved consistent, prolonged survival which highly correlated with reduced heart inflammation and DNA damage. Importantly, Lamin A treatment improved but could not reproduce long term survival, and Lamin A administration to healthy hearts itself induced DCM. Mechanistically, we identified this lapse as caused by a dose-dependent toxicity of Lamin A, which was independent from its maturation.

Conclusions: In vivo candidate evaluation revealed that supplementation of Lamin C or knockdown of Sun1 significantly suppressed Lmna DCM and achieve prolonged survival. Conversely, Lamin A supplementation did not rescue long term survival and may impart detrimental cardiotoxicity risk. This study highlights a potential of advancing Lamin C and Sun1 as therapeutic targets for the treatment of LMNA DCM.

Keywords: AAV; Dilated cardiomyopathy; Fibrosis; Gene therapy; Inflammation; Lamin A/C; Sun1.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Cardiomyopathies*
Cardiomyopathy, Dilated* / genetics
Cardiomyopathy, Dilated* / pathology
Fibrosis
Humans
Inflammation / complications
Lamin Type A / genetics
Lamin Type A / metabolism
Mutation
Transforming Growth Factor beta

Substances

Lamin Type A
Transforming Growth Factor beta
LMNA protein, human