4-Hydroxynonenal impairs miRNA maturation in heart failure via Dicer post-translational modification

Ligia A Kiyuna; Darlan S Candido; Luiz R G Bechara; Itamar C G Jesus; Lisley S Ramalho; Barbara Krum; Ruda P Albuquerque; Juliane C Campos; Luiz H M Bozi; Vanessa O Zambelli; Ariane N Alves; Nicolás Campolo; Mauricio Mastrogiovanni; Silvina Bartesaghi; Alejandro Leyva; Rosario Durán; Rafael Radi; Guilherme M Arantes; Edécio Cunha-Neto; Marcelo A Mori; Che-Hong Chen; Wenjin Yang; Daria Mochly-Rosen; Ian J MacRae; Ludmila R P Ferreira; Julio C B Ferreira

doi:10.1093/eurheartj/ehad662

4-Hydroxynonenal impairs miRNA maturation in heart failure via Dicer post-translational modification

Eur Heart J. 2023 Nov 21;44(44):4696-4712. doi: 10.1093/eurheartj/ehad662.

Authors

Ligia A Kiyuna¹, Darlan S Candido², Luiz R G Bechara¹, Itamar C G Jesus¹, Lisley S Ramalho¹, Barbara Krum¹, Ruda P Albuquerque¹, Juliane C Campos¹, Luiz H M Bozi¹, Vanessa O Zambelli³, Ariane N Alves⁴, Nicolás Campolo⁵, Mauricio Mastrogiovanni⁵, Silvina Bartesaghi⁵, Alejandro Leyva⁶, Rosario Durán⁶, Rafael Radi⁵, Guilherme M Arantes⁴, Edécio Cunha-Neto², Marcelo A Mori⁷, Che-Hong Chen⁸, Wenjin Yang⁹, Daria Mochly-Rosen⁸, Ian J MacRae¹⁰, Ludmila R P Ferreira^{2

11

12}, Julio C B Ferreira^{1

8}

Affiliations

¹ Department of Anatomy, Institute of Biomedical Sciences, University of Sao Paulo, Av. Prof. Lineu Prestes, 2415 - Butanta, 05508-000 São Paulo-SP, Brazil.
² Laboratory of Immunology, Heart Institute, University of São Paulo School of Medicine, São Paulo, Brazil.
³ Laboratory of Pain and Signaling, Butantan Institute, São Paulo, Brazil.
⁴ Department of Biochemistry, Institute of Chemistry, University of Sao Paulo, São Paulo, Brazil.
⁵ Departamento de Bioquímica and Centro de Investigaciones Biomédicas (CEINBIO), Facultad de Medicina, Universidad de la República (UdelaR), Montevideo, Uruguay.
⁶ Unidad de Bioquímica y Proteómica Analítica (UByPA), Instituto de Investigaciones Biológicas Celemente Estable & Institut Pasteur de Montevideo, Montevideo, Uruguay.
⁷ Department of Biochemistry and Tissue Biology, Institute of Biology, University of Campinas (Unicamp), São Paulo, Brazil.
⁸ Department of Chemical and Systems Biology, Stanford University School of Medicine, CCSR 3145A, 269 Campus Drive, Stanford, CA 94305, USA.
⁹ Foresee Pharmaceuticals, Co., Ltd, Taipei, Taiwan.
¹⁰ Department of Integrative Structural and Computational Biology, The Scripps Research Institute, La Jolla, CA, USA.
¹¹ Department of Morphology, Institute of Biological Sciences, Federal University of Minas Gerais, Minas Gerais, Brazil.
¹² Brazilian National Institute of Vaccine Science and Technology, Federal University of Minas Gerais, Minas Gerais, Brazil.

PMID: 37944136
DOI: 10.1093/eurheartj/ehad662

Abstract

Background and aims: Developing novel therapies to battle the global public health burden of heart failure remains challenging. This study investigates the underlying mechanisms and potential treatment for 4-hydroxynonenal (4-HNE) deleterious effects in heart failure.

Methods: Biochemical, functional, and histochemical measurements were applied to identify 4-HNE adducts in rat and human failing hearts. In vitro studies were performed to validate 4-HNE targets.

Results: 4-HNE, a reactive aldehyde by-product of mitochondrial dysfunction in heart failure, covalently inhibits Dicer, an RNase III endonuclease essential for microRNA (miRNA) biogenesis. 4-HNE inhibition of Dicer impairs miRNA processing. Mechanistically, 4-HNE binds to recombinant human Dicer through an intermolecular interaction that disrupts both activity and stability of Dicer in a concentration- and time-dependent manner. Dithiothreitol neutralization of 4-HNE or replacing 4-HNE-targeted residues in Dicer prevents 4-HNE inhibition of Dicer in vitro. Interestingly, end-stage human failing hearts from three different heart failure aetiologies display defective 4-HNE clearance, decreased Dicer activity, and miRNA biogenesis impairment. Notably, boosting 4-HNE clearance through pharmacological re-activation of mitochondrial aldehyde dehydrogenase 2 (ALDH2) using Alda-1 or its improved orally bioavailable derivative AD-9308 restores Dicer activity. ALDH2 is a major enzyme responsible for 4-HNE removal. Importantly, this response is accompanied by improved miRNA maturation and cardiac function/remodelling in a pre-clinical model of heart failure.

Conclusions: 4-HNE inhibition of Dicer directly impairs miRNA biogenesis in heart failure. Strikingly, decreasing cardiac 4-HNE levels through pharmacological ALDH2 activation is sufficient to re-establish Dicer activity and miRNA biogenesis; thereby representing potential treatment for patients with heart failure.

Keywords: Aldehyde; Cardiac diseases; Mitochondria; Oxidative stress; Therapy.

MeSH terms

Aldehyde Dehydrogenase, Mitochondrial / genetics
Aldehydes / metabolism
Aldehydes / pharmacology
Animals
Heart Failure*
Humans
MicroRNAs* / metabolism
Protein Processing, Post-Translational
Rats
Ribonuclease III / genetics
Ribonuclease III / metabolism

Substances

4-hydroxy-2-nonenal
MicroRNAs
Ribonuclease III
Aldehydes
ALDH2 protein, human
Aldehyde Dehydrogenase, Mitochondrial

Abstract

MeSH terms

Substances

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