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Serum opacity factor normalizes erythrocyte morphology in Scarb1(−/−) mice in an HDL-free cholesterol-dependent way

Compared with WT mice, HDL receptor-deficient (Scarb1(−/−)) mice have higher plasma levels of free cholesterol (FC)-rich HDL and exhibit multiple pathologies associated with a high mol% FC in ovaries, platelets, and erythrocytes, which are reversed by lowering HDL. Bacterial serum opacity factor (SO...

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Autores principales: Wang, Ziyi, Yelamanchili, Dedipya, Liu, Jing, Gotto, Antonio M., Rosales, Corina, Gillard, Baiba K., Pownall, Henry J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Biochemistry and Molecular Biology 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10641538/
https://www.ncbi.nlm.nih.gov/pubmed/37821077
http://dx.doi.org/10.1016/j.jlr.2023.100456
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author Wang, Ziyi
Yelamanchili, Dedipya
Liu, Jing
Gotto, Antonio M.
Rosales, Corina
Gillard, Baiba K.
Pownall, Henry J.
author_facet Wang, Ziyi
Yelamanchili, Dedipya
Liu, Jing
Gotto, Antonio M.
Rosales, Corina
Gillard, Baiba K.
Pownall, Henry J.
author_sort Wang, Ziyi
collection PubMed
description Compared with WT mice, HDL receptor-deficient (Scarb1(−/−)) mice have higher plasma levels of free cholesterol (FC)-rich HDL and exhibit multiple pathologies associated with a high mol% FC in ovaries, platelets, and erythrocytes, which are reversed by lowering HDL. Bacterial serum opacity factor (SOF) catalyzes the opacification of plasma by targeting and quantitatively converting HDL to neo HDL (HDL remnant), a cholesterol ester-rich microemulsion, and lipid-free APOA1. SOF delivery with an adeno-associated virus (AAV(SOF)) constitutively lowers plasma HDL-FC and reverses female infertility in Scarb1(−/−) mice in an HDL-dependent way. We tested whether AAV(SOF) delivery to Scarb1(−/−) mice will normalize erythrocyte morphology in an HDL-FC-dependent way. We determined erythrocyte morphology and FC content (mol%) in three groups—WT, untreated Scarb1(−/−) (control), and Scarb1(−/−) mice receiving AAV(SOF)—and correlated these with their respective HDL-mol% FC. Plasma-, HDL-, and tissue-lipid compositions were also determined. Plasma- and HDL-mol% FC positively correlated across all groups. Among Scarb1(−/−) mice, AAV(SOF) treatment normalized reticulocyte number, erythrocyte morphology, and erythrocyte-mol% FC. Erythrocyte-mol% FC positively correlated with HDL-mol% FC and with both the number of reticulocytes and abnormal erythrocytes. AAV(SOF) treatment also reduced FC of extravascular tissues to a lesser extent. HDL-FC spontaneously transfers from plasma HDL to cell membranes. AAV(SOF) treatment lowers erythrocyte-FC and normalizes erythrocyte morphology and lipid composition by reducing HDL-mol% FC.
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spelling pubmed-106415382023-11-14 Serum opacity factor normalizes erythrocyte morphology in Scarb1(−/−) mice in an HDL-free cholesterol-dependent way Wang, Ziyi Yelamanchili, Dedipya Liu, Jing Gotto, Antonio M. Rosales, Corina Gillard, Baiba K. Pownall, Henry J. J Lipid Res Research Article Compared with WT mice, HDL receptor-deficient (Scarb1(−/−)) mice have higher plasma levels of free cholesterol (FC)-rich HDL and exhibit multiple pathologies associated with a high mol% FC in ovaries, platelets, and erythrocytes, which are reversed by lowering HDL. Bacterial serum opacity factor (SOF) catalyzes the opacification of plasma by targeting and quantitatively converting HDL to neo HDL (HDL remnant), a cholesterol ester-rich microemulsion, and lipid-free APOA1. SOF delivery with an adeno-associated virus (AAV(SOF)) constitutively lowers plasma HDL-FC and reverses female infertility in Scarb1(−/−) mice in an HDL-dependent way. We tested whether AAV(SOF) delivery to Scarb1(−/−) mice will normalize erythrocyte morphology in an HDL-FC-dependent way. We determined erythrocyte morphology and FC content (mol%) in three groups—WT, untreated Scarb1(−/−) (control), and Scarb1(−/−) mice receiving AAV(SOF)—and correlated these with their respective HDL-mol% FC. Plasma-, HDL-, and tissue-lipid compositions were also determined. Plasma- and HDL-mol% FC positively correlated across all groups. Among Scarb1(−/−) mice, AAV(SOF) treatment normalized reticulocyte number, erythrocyte morphology, and erythrocyte-mol% FC. Erythrocyte-mol% FC positively correlated with HDL-mol% FC and with both the number of reticulocytes and abnormal erythrocytes. AAV(SOF) treatment also reduced FC of extravascular tissues to a lesser extent. HDL-FC spontaneously transfers from plasma HDL to cell membranes. AAV(SOF) treatment lowers erythrocyte-FC and normalizes erythrocyte morphology and lipid composition by reducing HDL-mol% FC. American Society for Biochemistry and Molecular Biology 2023-10-10 /pmc/articles/PMC10641538/ /pubmed/37821077 http://dx.doi.org/10.1016/j.jlr.2023.100456 Text en © 2023 The Authors https://creativecommons.org/licenses/by/4.0/This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Research Article
Wang, Ziyi
Yelamanchili, Dedipya
Liu, Jing
Gotto, Antonio M.
Rosales, Corina
Gillard, Baiba K.
Pownall, Henry J.
Serum opacity factor normalizes erythrocyte morphology in Scarb1(−/−) mice in an HDL-free cholesterol-dependent way
title Serum opacity factor normalizes erythrocyte morphology in Scarb1(−/−) mice in an HDL-free cholesterol-dependent way
title_full Serum opacity factor normalizes erythrocyte morphology in Scarb1(−/−) mice in an HDL-free cholesterol-dependent way
title_fullStr Serum opacity factor normalizes erythrocyte morphology in Scarb1(−/−) mice in an HDL-free cholesterol-dependent way
title_full_unstemmed Serum opacity factor normalizes erythrocyte morphology in Scarb1(−/−) mice in an HDL-free cholesterol-dependent way
title_short Serum opacity factor normalizes erythrocyte morphology in Scarb1(−/−) mice in an HDL-free cholesterol-dependent way
title_sort serum opacity factor normalizes erythrocyte morphology in scarb1(−/−) mice in an hdl-free cholesterol-dependent way
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10641538/
https://www.ncbi.nlm.nih.gov/pubmed/37821077
http://dx.doi.org/10.1016/j.jlr.2023.100456
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