Evaluation of the lipid-binding properties of recombinant dystrophin spectrin-like repeat domains R1-3
G Cooper-Olson, LR Rodino-Klapac… - Journal of …, 2021 - journals.sagepub.com
G Cooper-Olson, LR Rodino-Klapac, RA Potter
Journal of Neuromuscular Diseases, 2021•journals.sagepub.comRecombinant micro-dystrophin genes are designed to treat Duchenne muscular dystrophy
(DMD) by retaining dystrophin domains believed to play key functional roles while fitting the
packaging capacity of adeno-associated virus vectors. Domains R1-3 are important for
muscle force generation and for association with the sarcolemma, but the nature of this
interaction is not fully understood. We measured lipid-binding affinity of 3 peptides
containing different spectrin-like repeat modules (R1-3; R1-2; and R1, 2, 22). Lipid-binding …
(DMD) by retaining dystrophin domains believed to play key functional roles while fitting the
packaging capacity of adeno-associated virus vectors. Domains R1-3 are important for
muscle force generation and for association with the sarcolemma, but the nature of this
interaction is not fully understood. We measured lipid-binding affinity of 3 peptides
containing different spectrin-like repeat modules (R1-3; R1-2; and R1, 2, 22). Lipid-binding …
Recombinant micro-dystrophin genes are designed to treat Duchenne muscular dystrophy (DMD) by retaining dystrophin domains believed to play key functional roles while fitting the packaging capacity of adeno-associated virus vectors. Domains R1-3 are important for muscle force generation and for association with the sarcolemma, but the nature of this interaction is not fully understood. We measured lipid-binding affinity of 3 peptides containing different spectrin-like repeat modules (R1-3; R1-2; and R1, 2, 22). Lipid-binding affinity was highest with R1-3, suggesting that the complete R1-R3 region could be beneficial and should be considered for inclusion in micro-dystrophin constructs.
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