Your search keyword '"apolipoprotein mimetics"' showing total 6 results

1. Apolipoprotein A-I mimetics

Author

Reddy, Srinivasa T, Navab, Mohamad, Anantharamaiah, Gattadahalli M, and Fogelman, Alan M

Subjects

Biotechnology, Clinical Research, Cardiovascular, Atherosclerosis, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Animals, Apolipoprotein A-I, Biomimetics, Disease, Humans, Peptidomimetics, apolipoprotein mimetics, apolipoproteins, atherosclerosis, cancer, HDL, Medical Biochemistry and Metabolomics, Cardiorespiratory Medicine and Haematology, Clinical Sciences, Cardiovascular System & Hematology

Abstract

Purpose of reviewTo summarize recent publications in the field of apolipoprotein mimetics.Recent findingsApolipoprotein mimetic peptides continue to show efficacy in a number of animal models of disease and demonstrate properties that make them attractive as potential therapeutic agents. A number of new apolipoprotein mimetics have been described recently. A major site of action of apolipoprotein mimetic peptides was found to be in the small intestine in which they decrease the levels of proinflammatory bioactive lipids. A major problem related to the use of apolipoprotein mimetic peptides is their cost, particularly those that need to be generated by solid phase synthesis with chemical addition of end-blocking groups. Novel approaches to apolipoprotein mimetic therapy have emerged recently that show promise in overcoming these barriers.SummaryDespite the recent failure of therapies designed to raise HDL-cholesterol in humans, an approach to therapy using mimetics of HDL and its components continues to show promise.

Published

2014

2. Apolipoprotein-mimetic nanodiscs reduce lipid accumulation and improve liver function in acid sphingomyelinase deficiency.

Author

Halseth, Troy A., Correia, Adele B., Schultz, Mark L., Fawaz, Maria V., Kuiper, Esmée Q., Kumaran, Preethi, Dorsey, Kristen Hong, Schuchman, Edward H., Lieberman, Andrew P., and Schwendeman, Anna

Subjects

NIEMANN-Pick diseases, LIPIDOSES, APOLIPOPROTEIN A, HIGH density lipoproteins, PERIPHERAL circulation, LIPIDS

Abstract

Acid sphingomyelinase deficiency (ASMD) is a severe lipid storage disorder caused by the diminished activity of the acid sphingomyelinase enzyme. ASMD is characterized by the accumulation of sphingomyelin in late endosomes and lysosomes leading to progressive neurological dysfunction and hepatosplenomegaly. Our objective was to investigate the utility of synthetic apolipoprotein A-I (ApoA-I) mimetics designed to act as lipid scavengers for the treatment of ASMD. We determined the lead peptide, 22A, could reduce sphingomyelin accumulation in ASMD patient skin fibroblasts in a dose dependent manner. Intraperitoneal administration of 22A formulated as a synthetic high-density lipoprotein (sHDL) nanodisc mobilized sphingomyelin from peripheral tissues into circulation and improved liver function in a mouse model of ASMD. Together, our data demonstrates that apolipoprotein mimetics could serve as a novel therapeutic strategy for modulating the pathology observed in ASMD. Synthetic high-density lipoprotein nanodiscs accept excess sphingomyelin from peripheral tissues in a mouse model of ASMD. Created with BioRender.com [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

3. Apolipoprotein-mimetic nanodiscs reduce lipid accumulation and improve liver function in acid sphingomyelinase deficiency.

Author

Halseth TA, Correia AB, Schultz ML, Fawaz MV, Kuiper EQ, Kumaran P, Dorsey KH, Schuchman EH, Lieberman AP, and Schwendeman A

Subjects

Animals, Mice, Humans, Sphingomyelins, Peptides therapeutic use, Liver pathology, Niemann-Pick Disease, Type A drug therapy, Niemann-Pick Disease, Type A pathology

Abstract

Acid sphingomyelinase deficiency (ASMD) is a severe lipid storage disorder caused by the diminished activity of the acid sphingomyelinase enzyme. ASMD is characterized by the accumulation of sphingomyelin in late endosomes and lysosomes leading to progressive neurological dysfunction and hepatosplenomegaly. Our objective was to investigate the utility of synthetic apolipoprotein A-I (ApoA-I) mimetics designed to act as lipid scavengers for the treatment of ASMD. We determined the lead peptide, 22A, could reduce sphingomyelin accumulation in ASMD patient skin fibroblasts in a dose dependent manner. Intraperitoneal administration of 22A formulated as a synthetic high-density lipoprotein (sHDL) nanodisc mobilized sphingomyelin from peripheral tissues into circulation and improved liver function in a mouse model of ASMD. Together, our data demonstrates that apolipoprotein mimetics could serve as a novel therapeutic strategy for modulating the pathology observed in ASMD., Competing Interests: Declaration of competing interest Dr. Schwendeman declares financial interests for board membership, as a paid consultant, for research funding, and/or as equity holder in EVOQ Therapeutics. The University of Michigan has a financial interest in EVOQ Therapeutics, Inc., (Copyright © 2023. Published by Elsevier Inc.)

Published

2023

4. Mechanistic Insights into the Activation of Lecithin-Cholesterol Acyltransferase in Therapeutic Nanodiscs Composed of Apolipoprotein A-I Mimetic Peptides and Phospholipids

Author

Laura Giorgi, Akseli Niemelä, Esa-Pekka Kumpula, Ossi Natri, Petteri Parkkila, Juha T. Huiskonen, Artturi Koivuniemi, Faculty of Pharmacy, University of Helsinki, Division of Pharmaceutical Biosciences, Institute of Biotechnology, Helsinki Institute of Life Science HiLIFE, Joint Activities, Laboratory of Structural Biology, Department of Physics, Division of Pharmaceutical Chemistry and Technology, and Pharmaceutical biophysics group

Subjects

apolipoprotein mimetics, Apolipoprotein A-I, LECITHINCHOLESTEROL ACYLTRANSFERASE, Pharmaceutical Science, TRANSITIONS, reverse cholesterol transport, Phosphatidylcholine-Sterol O-Acyltransferase, DISCOIDAL COMPLEXES, Cholesterol, high-density lipoprotein (HDL), molecular dynamics simulation, SIZE, electron microscopy imaging, DOMAIN, 317 Pharmacy, Catalytic Domain, Drug Discovery, Lecithins, acyltransferase, HIGH-DENSITY-LIPOPROTEINS, Molecular Medicine, Lipoproteins, HDL, Peptides, Phospholipids, Sterol O-Acyltransferase

Abstract

The mechanistic details behind the activation of lecithin-cholesterol acyltransferase (LCAT) by apolipoprotein A-I (apoA-I) and its mimetic peptides are still enigmatic. Resolving the fundamental principles behind the LCAT activation will facilitate the design of advanced HDL-mimetic therapeutic nanodiscs for LCAT deficiencies and coronary heart disease, and for several targeted drug delivery applications. Here, we have combined coarse-grained molecular dynamics simulations with complementary experiments to gain mechanistic insight into how apoA-I mimetic peptide 22A and its variants attune LCAT activity in peptide-lipid nanodiscs. Results highlight that peptide 22A forms transient antiparallel dimers in the rim of nanodiscs. The dimerization tendency considerably decreases with the removal of C-terminal lysine K22, which has also been shown to reduce the cholesterol esterification activity of LCAT. In addition, our simulations revealed that LCAT prefers to localize to the rim of nanodiscs in a manner that shields the membrane-binding domain (MBD), αA-αA’, and the lid amino acids from the water phase, following the previous experimental evidence. Meanwhile, the location and conformation of LCAT in the rim of nanodisc are spatially more restricted when the active site covering lid of LCAT is in the open form. The average location and spatial dimensions of LCAT in its open form were highly compatible with the electron microscopy images. All peptide 22A variants studied here had a specific interaction site in the open LCAT structure flanked by the lid and MBD domain. The bound peptides showed different tendencies to form antiparallel dimers and, interestingly, the temporal binding site occupancies of the peptide variants affected their in vitro ability to promote LCAT-mediated cholesterol esterification.

Published

2022

5. Mechanistic Insights into the Activation of Lecithin-Cholesterol Acyltransferase in Therapeutic Nanodiscs Composed of Apolipoprotein A-I Mimetic Peptides and Phospholipids.

Author

Giorgi L, Niemelä A, Kumpula EP, Natri O, Parkkila P, Huiskonen JT, and Koivuniemi A

Subjects

Phospholipids metabolism, Lecithins, Sterol O-Acyltransferase metabolism, Lipoproteins, HDL chemistry, Catalytic Domain, Peptides, Cholesterol metabolism, Phosphatidylcholine-Sterol O-Acyltransferase chemistry, Phosphatidylcholine-Sterol O-Acyltransferase metabolism, Apolipoprotein A-I chemistry

Abstract

The mechanistic details behind the activation of lecithin-cholesterol acyltransferase (LCAT) by apolipoprotein A-I (apoA-I) and its mimetic peptides are still enigmatic. Resolving the fundamental principles behind LCAT activation will facilitate the design of advanced HDL-mimetic therapeutic nanodiscs for LCAT deficiencies and coronary heart disease and for several targeted drug delivery applications. Here, we have combined coarse-grained molecular dynamics simulations with complementary experiments to gain mechanistic insight into how apoA-Imimetic peptide 22A and its variants tune LCAT activity in peptide-lipid nanodiscs. Our results highlight that peptide 22A forms transient antiparallel dimers in the rim of nanodiscs. The dimerization tendency considerably decreases with the removal of C-terminal lysine K22, which has also been shown to reduce the cholesterol esterification activity of LCAT. In addition, our simulations revealed that LCAT prefers to localize to the rim of nanodiscs in a manner that shields the membrane-binding domain (MBD), αA-αA', and the lid amino acids from the water phase, following previous experimental evidence. Meanwhile, the location and conformation of LCAT in the rim of nanodiscs are spatially more restricted when the active site covering the lid of LCAT is in the open form. The average location and spatial dimensions of LCAT in its open form were highly compatible with the electron microscopy images. All peptide 22A variants studied here had a specific interaction site in the open LCAT structure flanked by the lid and MBD domain. The bound peptides showed different tendencies to form antiparallel dimers and, interestingly, the temporal binding site occupancies of the peptide variants affected their in vitro ability to promote LCAT-mediated cholesterol esterification.

Published

2022

6. Apolipoprotein A-I mimetics

Author

Mohamad Navab, Srinivasa T. Reddy, Alan M. Fogelman, and Gattadahalli M. Anantharamaiah

Subjects

apolipoprotein mimetics, HDL, Apolipoprotein B, Endocrinology, Diabetes and Metabolism, Clinical Sciences, Computational biology, Medical Biochemistry and Metabolomics, Cardiorespiratory Medicine and Haematology, Cardiovascular, Article, Biomimetics, Clinical Research, Genetics, Animals, Humans, cancer, Medicine, Disease, Molecular Biology, Nutrition and Dietetics, Apolipoprotein A-I, biology, business.industry, Extramural, Cell Biology, Atherosclerosis, Cardiovascular System & Hematology, 5.1 Pharmaceuticals, biology.protein, Peptidomimetics, Development of treatments and therapeutic interventions, Cardiology and Cardiovascular Medicine, business, apolipoproteins, Biotechnology

Abstract

Purpose of reviewTo summarize recent publications in the field of apolipoprotein mimetics.Recent findingsApolipoprotein mimetic peptides continue to show efficacy in a number of animal models of disease and demonstrate properties that make them attractive as potential therapeutic agents. A number of new apolipoprotein mimetics have been described recently. A major site of action of apolipoprotein mimetic peptides was found to be in the small intestine in which they decrease the levels of proinflammatory bioactive lipids. A major problem related to the use of apolipoprotein mimetic peptides is their cost, particularly those that need to be generated by solid phase synthesis with chemical addition of end-blocking groups. Novel approaches to apolipoprotein mimetic therapy have emerged recently that show promise in overcoming these barriers.SummaryDespite the recent failure of therapies designed to raise HDL-cholesterol in humans, an approach to therapy using mimetics of HDL and its components continues to show promise.

Published

2014