Pemafibrate Protects against Fatty Acid-Induced Nephropathy by Maintaining Renal Fatty Acid Metabolism

被引:11
作者
Aomura, Daiki [1 ]
Harada, Makoto [1 ]
Yamada, Yosuke [1 ]
Nakajima, Takero [2 ]
Hashimoto, Koji [1 ]
Tanaka, Naoki [2 ,3 ]
Kamijo, Yuji [1 ]
机构
[1] Shinshu Univ, Dept Nephrol, Sch Med, Matsumoto, Nagano 3908621, Japan
[2] Shinshu Univ, Dept Metab Regulat, Sch Med, Matsumoto, Nagano 3908621, Japan
[3] Shinshu Univ, Int Relat Off, Sch Med, Matsumoto, Nagano 3908621, Japan
来源
METABOLITES | 2021年 / 11卷 / 06期
关键词
pemafibrate; peroxisomal proliferator-activated receptor alpha; renal fatty acid metabolism; lipotoxicity; nephrology; ACTIVATED RECEPTOR-ALPHA; MODULATOR SPPARM-ALPHA; DYSLIPIDEMIC PATIENTS; DOUBLE-BLIND; KIDNEY; K-877; MICE; PURIFICATION; LIVER; FENOFIBRATE;
D O I
10.3390/metabo11060372
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
As classical agonists for peroxisomal proliferator-activated receptor alpha (PPAR alpha), fibrates activate renal fatty acid metabolism (FAM) and provide renoprotection. However, fibrate prescription is limited in patients with kidney disease, since impaired urinary excretion of the drug causes serious adverse effects. Pemafibrate (PEM), a novel selective PPAR alpha modulator, is mainly excreted in bile, and, thus, may be safe and effective in kidney disease patients. It remains unclear, however, whether PEM actually exhibits renoprotective properties. We investigated this issue using mice with fatty acid overload nephropathy (FAON). PEM (0.5 mg/kg body weight/day) or a vehicle was administered for 20 days to 13-week-old wild-type male mice, which were simultaneously injected with free fatty acid (FFA)-binding bovine serum albumin from day 7 to day 20 to induce FAON. All mice were sacrificed on day 20 for assessment of the renoprotective effect of PEM against FAON. PEM significantly attenuated the histological findings of tubular injury caused by FAON, increased the renal expressions of mRNA and proteins related to FAM, and decreased renal FFA content and oxidative stress. Taken together, PEM exhibits renoprotective effects through the activation and maintenance of renal FAM and represents a promising drug for kidney disease.
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页数:13
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共 42 条
[11]   COMPLETE NUCLEOTIDE-SEQUENCE OF CDNA AND DEDUCED AMINO-ACID-SEQUENCE OF RAT-LIVER CATALASE [J].
FURUTA, S ;
HAYASHI, H ;
HIJIKATA, M ;
MIYAZAWA, S ;
OSUMI, T ;
HASHIMOTO, T .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1986, 83 (02) :313-317
[12]   Peroxisome proliferator-activated receptor α-dependent renoprotection of murine kidney by irbesartan [J].
Harada, Makoto ;
Kamijo, Yuji ;
Nakajima, Takero ;
Hashimoto, Koji ;
Yamada, Yosuke ;
Shimojo, Hisashi ;
Gonzalez, Frank J. ;
Aoyama, Toshifumi .
CLINICAL SCIENCE, 2016, 130 (21) :1969-1981
[13]   PPARα Activation Protects against Anti-Thy1 Nephritis by Suppressing Glomerular NF-κB Signaling [J].
Hashimoto, Koji ;
Kamijo, Yuji ;
Nakajima, Takero ;
Harada, Makoto ;
Higuchi, Makoto ;
Ehara, Takashi ;
Shigematsu, Hidekazu ;
Aoyama, Toshifumi .
PPAR RESEARCH, 2012, 2012
[14]   Efficacy and safety of pemafibrate (K-877), a selective peroxisome proliferator-activated receptor α modulator, in patients with dyslipidemia: Results from a 24-week, randomized, double blind, active-controlled, phase 3 trial [J].
Ishibashi, Shun ;
Arai, Hidenori ;
Yokote, Koutaro ;
Araki, Eiichi ;
Suganami, Hideki ;
Yamashita, Shizuya .
JOURNAL OF CLINICAL LIPIDOLOGY, 2018, 12 (01) :173-184
[15]   Effects of K-877, a novel selective PPARα modulator (SPPARMα), in dyslipidaemic patients: A randomized, double blind, active- and placebo-controlled, phase 2 trial [J].
Ishibashi, Shun ;
Yamashita, Shizuya ;
Arai, Hidenori ;
Araki, Eiichi ;
Yokote, Koutaro ;
Suganami, Hideki ;
Fruchart, Jean-Charles ;
Kodama, Tatsuhiko .
ATHEROSCLEROSIS, 2016, 249 :36-43
[16]   Effects of Fibrates in Kidney Disease [J].
Jun, Min ;
Zhu, Bin ;
Tonelli, Marcello ;
Jardine, Meg J. ;
Patel, Anushka ;
Neal, Bruce ;
Liyanage, Thaminda ;
Keech, Anthony ;
Cass, Alan ;
Perkovic, Vlado .
JOURNAL OF THE AMERICAN COLLEGE OF CARDIOLOGY, 2012, 60 (20) :2061-2071
[17]   Urinary free fatty acids bound to albumin aggravate tubulointerstitial damage [J].
Kamijo, A ;
Kimura, K ;
Sugaya, T ;
Yamanouchi, M ;
Hase, H ;
Kaneko, T ;
Hirata, Y ;
Goto, A ;
Fujita, T ;
Omata, M .
KIDNEY INTERNATIONAL, 2002, 62 (05) :1628-1637
[18]   Identification of functions of peroxisome proliferator-activated receptor α in proximal tubules [J].
Kamijo, Y ;
Hora, K ;
Tanaka, N ;
Usuda, N ;
Kiyosawa, K ;
Nakajima, T ;
Gonzalez, FJ ;
Aoyama, T .
JOURNAL OF THE AMERICAN SOCIETY OF NEPHROLOGY, 2002, 13 (07) :1691-1702
[19]   PPARα protects proximal tubular cells from acute fatty acid toxicity [J].
Kamijo, Yuji ;
Hora, Kazuhiko ;
Kono, Keiichi ;
Takahashi, Kyoko ;
Higuchi, Makoto ;
Ehara, Takashi ;
Kiyosawa, Kendo ;
Shigematsu, Hidekazu ;
Gonzalez, Frank J. ;
Aoyama, Toshifumi .
JOURNAL OF THE AMERICAN SOCIETY OF NEPHROLOGY, 2007, 18 (12) :3089-3100
[20]   Defective fatty acid oxidation in renal tubular epithelial cells has a key role in kidney fibrosis development [J].
Kang, Hyun Mi ;
Ahn, Seon Ho ;
Choi, Peter ;
Ko, Yi-An ;
Han, Seung Hyeok ;
Chinga, Frank ;
Park, Ae Seo Deok ;
Tao, Jian Ling ;
Sharma, Kumar ;
Pullman, James ;
Bottinger, Erwin P. ;
Goldberg, Ira J. ;
Susztak, Katalin .
NATURE MEDICINE, 2015, 21 (01) :37-46
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