Identification of Differential Roles of MicroRNA‐33a and ‐33b During Atherosclerosis Progression With Genetically Modified Mice

BACKGROUND: MicroRNA (miR)‐33 targets cholesterol transporter ATP‐binding cassette protein A1 and other antiatherogenic targets and contributes to atherogenic progression. Its inhibition or deletion is known to result in the amelioration of atherosclerosis in mice. However, mice lack the other membe...

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Autores principales: Koyama, Satoshi, Horie, Takahiro, Nishino, Tomohiro, Baba, Osamu, Sowa, Naoya, Miyasaka, Yui, Kuwabara, Yasuhide, Nakao, Tetsushi, Nishiga, Masataka, Nishi, Hitoo, Nakashima, Yasuhiro, Nakazeki, Fumiko, Ide, Yuya, Kimura, Masahiro, Tsuji, Shuhei, Ruiz Rodriguez, Randolph, Xu, Sijia, Yamasaki, Tomohiro, Otani, Chiharu, Watanabe, Toshimitsu, Nakamura, Tomoyuki, Hasegawa, Koji, Kimura, Takeshi, Ono, Koh
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2019
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6662357/
https://www.ncbi.nlm.nih.gov/pubmed/31242815
http://dx.doi.org/10.1161/JAHA.119.012609
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author Koyama, Satoshi
Horie, Takahiro
Nishino, Tomohiro
Baba, Osamu
Sowa, Naoya
Miyasaka, Yui
Kuwabara, Yasuhide
Nakao, Tetsushi
Nishiga, Masataka
Nishi, Hitoo
Nakashima, Yasuhiro
Nakazeki, Fumiko
Ide, Yuya
Kimura, Masahiro
Tsuji, Shuhei
Ruiz Rodriguez, Randolph
Xu, Sijia
Yamasaki, Tomohiro
Otani, Chiharu
Watanabe, Toshimitsu
Nakamura, Tomoyuki
Hasegawa, Koji
Kimura, Takeshi
Ono, Koh
author_facet Koyama, Satoshi
Horie, Takahiro
Nishino, Tomohiro
Baba, Osamu
Sowa, Naoya
Miyasaka, Yui
Kuwabara, Yasuhide
Nakao, Tetsushi
Nishiga, Masataka
Nishi, Hitoo
Nakashima, Yasuhiro
Nakazeki, Fumiko
Ide, Yuya
Kimura, Masahiro
Tsuji, Shuhei
Ruiz Rodriguez, Randolph
Xu, Sijia
Yamasaki, Tomohiro
Otani, Chiharu
Watanabe, Toshimitsu
Nakamura, Tomoyuki
Hasegawa, Koji
Kimura, Takeshi
Ono, Koh
author_sort Koyama, Satoshi
collection PubMed
description BACKGROUND: MicroRNA (miR)‐33 targets cholesterol transporter ATP‐binding cassette protein A1 and other antiatherogenic targets and contributes to atherogenic progression. Its inhibition or deletion is known to result in the amelioration of atherosclerosis in mice. However, mice lack the other member of the miR‐33 family, miR‐33b, which exists in humans and other large mammals. Thus, precise evaluation and comparison of the responsibilities of these 2 miRs during the progression of atherosclerosis has not been reported, although they are essential. METHODS AND RESULTS: In this study, we performed a comprehensive analysis of the difference between the function of miR‐33a and miR‐33b using genetically modified mice. We generated 4 strains with or without miR‐33a and miR‐33b. Comparison between mice with only miR‐33a (wild‐type mice) and mice with only miR‐33b (miR‐33a(−/−)/miR‐33b(+/+)) revealed the dominant expression of miR‐33b in the liver. To evaluate the whole body atherogenic potency of miR‐33a and miR‐33b, we developed apolipoprotein E–deficient/miR‐33a(+/+)/miR‐33b(−/−) mice and apolipoprotein E–deficient/miR‐33a(−/−)/miR‐33b(+/+) mice. With a high‐fat and high‐cholesterol diet, the apolipoprotein E–deficient/miR‐33a(−/−)/miR‐33b(+/+) mice developed increased atherosclerotic plaque versus apolipoprotein E–deficient/miR‐33a(+/+)/miR‐33b(−/−) mice, in line with the predominant expression of miR‐33b in the liver and worsened serum cholesterol profile. By contrast, a bone marrow transplantation study showed no significant difference, which was consistent with the relevant expression levels of miR‐33a and miR‐33b in bone marrow cells. CONCLUSIONS: The miR‐33 family exhibits differences in distribution and regulation and particularly in the progression of atherosclerosis; miR‐33b would be more potent than miR‐33a.
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spelling pubmed-66623572019-08-02 Identification of Differential Roles of MicroRNA‐33a and ‐33b During Atherosclerosis Progression With Genetically Modified Mice Koyama, Satoshi Horie, Takahiro Nishino, Tomohiro Baba, Osamu Sowa, Naoya Miyasaka, Yui Kuwabara, Yasuhide Nakao, Tetsushi Nishiga, Masataka Nishi, Hitoo Nakashima, Yasuhiro Nakazeki, Fumiko Ide, Yuya Kimura, Masahiro Tsuji, Shuhei Ruiz Rodriguez, Randolph Xu, Sijia Yamasaki, Tomohiro Otani, Chiharu Watanabe, Toshimitsu Nakamura, Tomoyuki Hasegawa, Koji Kimura, Takeshi Ono, Koh J Am Heart Assoc Original Research BACKGROUND: MicroRNA (miR)‐33 targets cholesterol transporter ATP‐binding cassette protein A1 and other antiatherogenic targets and contributes to atherogenic progression. Its inhibition or deletion is known to result in the amelioration of atherosclerosis in mice. However, mice lack the other member of the miR‐33 family, miR‐33b, which exists in humans and other large mammals. Thus, precise evaluation and comparison of the responsibilities of these 2 miRs during the progression of atherosclerosis has not been reported, although they are essential. METHODS AND RESULTS: In this study, we performed a comprehensive analysis of the difference between the function of miR‐33a and miR‐33b using genetically modified mice. We generated 4 strains with or without miR‐33a and miR‐33b. Comparison between mice with only miR‐33a (wild‐type mice) and mice with only miR‐33b (miR‐33a(−/−)/miR‐33b(+/+)) revealed the dominant expression of miR‐33b in the liver. To evaluate the whole body atherogenic potency of miR‐33a and miR‐33b, we developed apolipoprotein E–deficient/miR‐33a(+/+)/miR‐33b(−/−) mice and apolipoprotein E–deficient/miR‐33a(−/−)/miR‐33b(+/+) mice. With a high‐fat and high‐cholesterol diet, the apolipoprotein E–deficient/miR‐33a(−/−)/miR‐33b(+/+) mice developed increased atherosclerotic plaque versus apolipoprotein E–deficient/miR‐33a(+/+)/miR‐33b(−/−) mice, in line with the predominant expression of miR‐33b in the liver and worsened serum cholesterol profile. By contrast, a bone marrow transplantation study showed no significant difference, which was consistent with the relevant expression levels of miR‐33a and miR‐33b in bone marrow cells. CONCLUSIONS: The miR‐33 family exhibits differences in distribution and regulation and particularly in the progression of atherosclerosis; miR‐33b would be more potent than miR‐33a. John Wiley and Sons Inc. 2019-06-27 /pmc/articles/PMC6662357/ /pubmed/31242815 http://dx.doi.org/10.1161/JAHA.119.012609 Text en © 2019 The Authors. Published on behalf of the American Heart Association, Inc., by Wiley. This is an open access article under the terms of the http://creativecommons.org/licenses/by-nc-nd/4.0/ License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non‐commercial and no modifications or adaptations are made.
spellingShingle Original Research
Koyama, Satoshi
Horie, Takahiro
Nishino, Tomohiro
Baba, Osamu
Sowa, Naoya
Miyasaka, Yui
Kuwabara, Yasuhide
Nakao, Tetsushi
Nishiga, Masataka
Nishi, Hitoo
Nakashima, Yasuhiro
Nakazeki, Fumiko
Ide, Yuya
Kimura, Masahiro
Tsuji, Shuhei
Ruiz Rodriguez, Randolph
Xu, Sijia
Yamasaki, Tomohiro
Otani, Chiharu
Watanabe, Toshimitsu
Nakamura, Tomoyuki
Hasegawa, Koji
Kimura, Takeshi
Ono, Koh
Identification of Differential Roles of MicroRNA‐33a and ‐33b During Atherosclerosis Progression With Genetically Modified Mice
title Identification of Differential Roles of MicroRNA‐33a and ‐33b During Atherosclerosis Progression With Genetically Modified Mice
title_full Identification of Differential Roles of MicroRNA‐33a and ‐33b During Atherosclerosis Progression With Genetically Modified Mice
title_fullStr Identification of Differential Roles of MicroRNA‐33a and ‐33b During Atherosclerosis Progression With Genetically Modified Mice
title_full_unstemmed Identification of Differential Roles of MicroRNA‐33a and ‐33b During Atherosclerosis Progression With Genetically Modified Mice
title_short Identification of Differential Roles of MicroRNA‐33a and ‐33b During Atherosclerosis Progression With Genetically Modified Mice
title_sort identification of differential roles of microrna‐33a and ‐33b during atherosclerosis progression with genetically modified mice
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6662357/
https://www.ncbi.nlm.nih.gov/pubmed/31242815
http://dx.doi.org/10.1161/JAHA.119.012609
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