机构地区:[1]Department of Biomedical Engineering,Wisconsin Institute for Discovery,University of Wisconsin-Madison,Madison,WI,53715,USA [2]Department of Ophthalmology and Visual Sciences,University of Wisconsin-Madison,Madison,WI,53715,USA [3]Department of Surgery,School of Medicine,University of Virginia,Charlottesville,VA,22908,USA [4]The Biomedical Sciences Graduate Program(BIMS),School of Medicine,University of Virginia,Charlottesville,VA,22908,USA [5]Department of Biomedical Engineering,School of Engineering,University of Virginia,Charlottesville,VA,22908,USA [6]School of Medicine and Health Sciences,George Washington University,Washington,DC,20052,USA [7]Department of Cardiac Surgery,Michigan Medicine,University of Michigan,Ann Arbor,MI,48109,USA
出 处:《Bioactive Materials》2023年第8期52-63,共12页生物活性材料(英文)
基 金:supported by the National Institute of Health(NIH)grants R01HL133665(to L.-W.G.),R01HL143469;R01HL129785(to K.C.K,S.G.,and L.-W.G.);R01HL162895(to B.W.);R01HL132395 and 1S10RR027333(to J.A.H.);Overseas Research Fellowships,The Uehara Memorial Foundation in Japan(to T.S.).
摘 要:Abdominal aortic aneurysm(AAA)is a progressive aortic dilatation,causing~80%mortality upon rupture.Currently,there is no approved drug therapy for AAA.Surgical repairs are invasive and risky and thus not recommended to patients with small AAAs which,however,account for~90%of the newly diagnosed cases.It is therefore a compelling unmet clinical need to discover effective non-invasive strategies to prevent or slow down AAA progression.We contend that the first AAA drug therapy will only arise through discoveries of both effective drug targets and innovative delivery methods.There is substantial evidence that degenerative smooth muscle cells(SMCs)orchestrate AAA pathogenesis and progression.In this study,we made an exciting finding that PERK,the endoplasmic reticulum(ER)stress Protein Kinase R-like ER Kinase,is a potent driver of SMC degeneration and hence a potential therapeutic target.Indeed,local knockdown of PERK in elastase-challenged aorta significantly attenuated AAA lesions in vivo.In parallel,we also conceived a biomimetic nanocluster(NC)design uniquely tailored to AAA-targeting drug delivery.This NC demonstrated excellent AAA homing via a platelet-derived biomembrane coating;and when loaded with a selective PERK inhibitor(PERKi,GSK2656157),the NC therapy conferred remarkable benefits in both preventing aneurysm development and halting the progression of pre-existing aneurysmal lesions in two distinct rodent models of AAA.In summary,our current study not only establishes a new intervention target for mitigating SMC degeneration and aneurysmal pathogenesis,but also provides a powerful tool to facilitate the development of effective drug therapy of AAA.
关 键 词:Abdominal aortic aneurysm ER stress PERK Biomimetic nanomedicine Targeted delivery
分 类 号:TB383.1[一般工业技术—材料科学与工程]
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