TY - JOUR
T1 - AAV-based gene therapy prevents and halts the progression of dilated cardiomyopathy in a mouse model of phosphoglucomutase 1 deficiency (PGM1-CDG)
AU - Balakrishnan, Bijina
AU - Altassan, Ruqaiah
AU - Budhraja, Rohit
AU - Liou, Willisa
AU - Lupo, Arielle
AU - Bryant, Sarah
AU - Mankouski, Anastasiya
AU - Radenkovic, Silvia
AU - Preston, Graeme J.
AU - Pandey, Akhilesh
AU - Boudina, Sihem
AU - Kozicz, Tamas
AU - Morava-Kozicz, Eva
AU - Lai, Kent
N1 - Funding Information:
E.M. & T.K. are supported by the grant entitled Frontiers in Congenital Disorders of Glycosylation ( 1U54NS115198-01 ) from the National Institute of Neurological Diseases and Stroke ( NINDS ) and the National Center for Advancing Translational Sciences ( NCATS ), National Institute of Child Health and Human Development and the Rare Disorders Clinical Research Network ( RDCRN ), at the National Institute of Health.
Funding Information:
A.P. was funded by a grant from the NCI to the Mayo Clinic Comprehensive Cancer Center (NCI P30 CA15083).S.B. is supported by the National Heart, Lung, and Blood Institute (NHLBI) grant R01HL149870-01A1, the National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK) grant R01DK128819-01), and University of Utah Office of Vice-President of Research seed grant.E.M. & T.K. are supported by the grant entitled Frontiers in Congenital Disorders of Glycosylation (1U54NS115198-01) from the National Institute of Neurological Diseases and Stroke (NINDS) and the National Center for Advancing Translational Sciences (NCATS), National Institute of Child Health and Human Development and the Rare Disorders Clinical Research Network (RDCRN), at the National Institute of Health.K.L. is supported by the Eunice Kennedy Shriver National Institute of Child Health and Human Development grants (R01HD089933, R21HD104056), (FCDGC) Feasibility and Pilot Grant, University of Utah College of Pharmacy and Center for Genomic Medicine Therapeutic Catalyst Grant, and University of Utah Office of Vice-President of Research seed grant.
Funding Information:
K.L. is supported by the Eunice Kennedy Shriver National Institute of Child Health and Human Development grants (R01HD089933, R21HD104056 ), ( FCDGC ) Feasibility and Pilot Grant, University of Utah College of Pharmacy and Center for Genomic Medicine Therapeutic Catalyst Grant, and University of Utah Office of Vice-President of Research seed grant.
Funding Information:
A.P. was funded by a grant from the NCI to the Mayo Clinic Comprehensive Cancer Center ( NCI P30 CA15083 ).
Funding Information:
S.B. is supported by the National Heart, Lung, and Blood Institute ( NHLBI ) grant R01HL149870-01A1 , the National Institute of Diabetes and Digestive and Kidney Diseases ( NIDDK ) grant R01DK128819-01 ), and University of Utah Office of Vice-President of Research seed grant.
Publisher Copyright:
© 2023 Elsevier Inc.
PY - 2023
Y1 - 2023
N2 - Phosphoglucomutase 1 (PGM1) deficiency is recognized as the third most common N-linked congenital disorders of glycosylation (CDG) in humans. Affected individuals present with liver, musculoskeletal, endocrine, and coagulation symptoms; however, the most life-threatening complication is the early onset of dilated cardiomyopathy (DCM). Recently, we discovered that oral D-galactose supplementation improved liver disease, endocrine, and coagulation abnormalities, but does not alleviate the fatal cardiomyopathy and the associated myopathy. Here we report on left ventricular ejection fraction (LVEF) in 6 individuals with PGM1-CDG. LVEF was pathologically low in most of these individuals and varied between 10% and 65%. To study the pathobiology of the cardiac disease observed in PGM1-CDG, we constructed a novel cardiomyocyte-specific conditional Pgm2 gene (mouse ortholog of human PGM1) knockout (Pgm2 cKO) mouse model. Echocardiography studies corroborated a DCM phenotype with significantly reduced ejection fraction and left ventricular dilation similar to those seen in individuals with PGM1-CDG. Histological studies demonstrated excess glycogen accumulation and fibrosis, while ultrastructural analysis revealed Z-disk disarray and swollen/fragmented mitochondria, which was similar to the ultrastructural pathology in the cardiac explant of an individual with PGM1-CDG. In addition, we found decreased mitochondrial function in the heart of KO mice. Transcriptomic analysis of hearts from mutant mice demonstrated a gene signature of DCM. Although proteomics revealed only mild changes in global protein expression in left ventricular tissue of mutant mice, a glycoproteomic analysis unveiled broad glycosylation changes with significant alterations in sarcolemmal proteins including different subunits of laminin-211, which was confirmed by immunoblot analyses. Finally, augmentation of PGM1 in KO mice via AAV9-PGM1 gene replacement therapy prevented and halted the progression of the DCM phenotype.
AB - Phosphoglucomutase 1 (PGM1) deficiency is recognized as the third most common N-linked congenital disorders of glycosylation (CDG) in humans. Affected individuals present with liver, musculoskeletal, endocrine, and coagulation symptoms; however, the most life-threatening complication is the early onset of dilated cardiomyopathy (DCM). Recently, we discovered that oral D-galactose supplementation improved liver disease, endocrine, and coagulation abnormalities, but does not alleviate the fatal cardiomyopathy and the associated myopathy. Here we report on left ventricular ejection fraction (LVEF) in 6 individuals with PGM1-CDG. LVEF was pathologically low in most of these individuals and varied between 10% and 65%. To study the pathobiology of the cardiac disease observed in PGM1-CDG, we constructed a novel cardiomyocyte-specific conditional Pgm2 gene (mouse ortholog of human PGM1) knockout (Pgm2 cKO) mouse model. Echocardiography studies corroborated a DCM phenotype with significantly reduced ejection fraction and left ventricular dilation similar to those seen in individuals with PGM1-CDG. Histological studies demonstrated excess glycogen accumulation and fibrosis, while ultrastructural analysis revealed Z-disk disarray and swollen/fragmented mitochondria, which was similar to the ultrastructural pathology in the cardiac explant of an individual with PGM1-CDG. In addition, we found decreased mitochondrial function in the heart of KO mice. Transcriptomic analysis of hearts from mutant mice demonstrated a gene signature of DCM. Although proteomics revealed only mild changes in global protein expression in left ventricular tissue of mutant mice, a glycoproteomic analysis unveiled broad glycosylation changes with significant alterations in sarcolemmal proteins including different subunits of laminin-211, which was confirmed by immunoblot analyses. Finally, augmentation of PGM1 in KO mice via AAV9-PGM1 gene replacement therapy prevented and halted the progression of the DCM phenotype.
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U2 - 10.1016/j.trsl.2023.01.004
DO - 10.1016/j.trsl.2023.01.004
M3 - Article
C2 - 36709920
AN - SCOPUS:85148765193
SN - 1931-5244
VL - 257
SP - 1
EP - 14
JO - Translational Research
JF - Translational Research
ER -