Defective heart chamber growth and myofibrillogenesis after knockout of<i>adprhl1</i>gene function by targeted disruption of the ancestral catalytic active site

Smith, Stuart J.; Towers, Norma; Demetriou, Kim; Mohun, Timothy J.

doi:10.1101/2020.02.13.947424

2020

DOI: 10.1101/2020.02.13.947424

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Defective heart chamber growth and myofibrillogenesis after knockout ofadprhl1gene function by targeted disruption of the ancestral catalytic active site

Stuart J. Smith

Norma Towers

Kim Demetriou

et al.

Abstract: 1 Cardiac adprhl1 CRISPR knockout Smith et al. Mohun Highlights.Comparison of adprhl1 morpholinos. Knockdown of the two Xenopus cardiac Adprhl1 protein species (40 and 23 kDa) causes failure of ventricle outgrowth. CRISPR/Cas9 targeted gene mutation of adprhl1 with multiple gRNAs reveals exonic locations that encode critical amino acids for Adprhl1 function.Repair of DSBs at exon 6 yields small in-frame deletions that cause specific ventricle myofibril assembly defects.The deletions disturb a conserved di-argi… Show more

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Cited by 2 publications

References 58 publications

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ARH Family of ADP-Ribose-Acceptor Hydrolases

Ishiwata-Endo

Katō

Yamashita

et al. 2022

Cells

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The ARH family of ADP-ribose-acceptor hydrolases consists of three 39-kDa members (ARH1-3), with similarities in amino acid sequence. ARH1 was identified based on its ability to cleave ADP-ribosyl-arginine synthesized by cholera toxin. Mammalian ADP-ribosyltransferases (ARTCs) mimicked the toxin reaction, with ARTC1 catalyzing the synthesis of ADP-ribosyl-arginine. ADP-ribosylation of arginine was stereospecific, with β-NAD+ as substrate and, α-anomeric ADP-ribose-arginine the reaction product. ARH1 hydrolyzed α-ADP-ribose-arginine, in addition to α-NAD+ and O-acetyl-ADP-ribose. Thus, ADP-ribose attached to oxygen-containing or nitrogen-containing functional groups was a substrate. Arh1 heterozygous and knockout (KO) mice developed tumors. Arh1-KO mice showed decreased cardiac contractility and developed myocardial fibrosis. In addition to Arh1-KO mice showed increased ADP-ribosylation of tripartite motif-containing protein 72 (TRIM72), a membrane-repair protein. ARH3 cleaved ADP-ribose from ends of the poly(ADP-ribose) (PAR) chain and released the terminal ADP-ribose attached to (serine)protein. ARH3 also hydrolyzed α-NAD+ and O-acetyl-ADP-ribose. Incubation of Arh3-KO cells with H2O2 resulted in activation of poly-ADP-ribose polymerase (PARP)-1, followed by increased nuclear PAR, increased cytoplasmic PAR, leading to release of Apoptosis Inducing Factor (AIF) from mitochondria. AIF, following nuclear translocation, stimulated endonucleases, resulting in cell death by Parthanatos. Human ARH3-deficiency is autosomal recessive, rare, and characterized by neurodegeneration and early death. Arh3-KO mice developed increased brain infarction following ischemia-reperfusion injury, which was reduced by PARP inhibitors. Similarly, PARP inhibitors improved survival of Arh3-KO cells treated with H2O2. ARH2 protein did not show activity in the in vitro assays described above for ARH1 and ARH3. ARH2 has a restricted tissue distribution, with primary involvement of cardiac and skeletal muscle. Overall, the ARH family has unique functions in biological processes and different enzymatic activities.

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ARH Family of ADP-Ribose-Acceptor Hydrolases

Ishiwata-Endo

Katō

Yamashita

et al. 2022

Cells

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Use of Frogs as a Model to Study the Etiology of HLHS

Nie

2023

JCDD

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A frog is a classical model organism used to uncover processes and regulations of early vertebrate development, including heart development. Recently, we showed that a frog also represents a useful model to study a rare human congenital heart disease, hypoplastic left heart syndrome. In this review, we first summarized the cellular events and molecular regulations of vertebrate heart development, and the benefit of using a frog model to study congenital heart diseases. Next, we described the challenges in elucidating the etiology of hypoplastic left heart syndrome and discussed how a frog model may contribute to our understanding of the molecular and cellular bases of the disease. We concluded that a frog model offers its unique advantage in uncovering the cellular mechanisms of hypoplastic left heart syndrome; however, combining multiple model organisms, including frogs, is needed to gain a comprehensive understanding of the disease.

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Defective heart chamber growth and myofibrillogenesis after knockout ofadprhl1gene function by targeted disruption of the ancestral catalytic active site

Cited by 2 publications

References 58 publications

ARH Family of ADP-Ribose-Acceptor Hydrolases

ARH Family of ADP-Ribose-Acceptor Hydrolases

Use of Frogs as a Model to Study the Etiology of HLHS

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