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      저항훈련은 랫 골격근에서 finasteride에 의해 유도된 단백질 항상성 교란을 개선시킨다 = Resistance Training Ameliorates Finasteride-Induced Disturbance in Protein Homeostasis in Skeletal Muscle of Rats

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      https://www.riss.kr/link?id=A106238791

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      다국어 초록 (Multilingual Abstract)

      PURPOSE: Finasteride is a competitive inhibitor of 5-alpha reductase type 2 enzyme that is commonly used to treat benign prostatic hyperplasia and male pattern hair loss. It is not clear about the synergistic effects of finasteride and resistance trai...

      PURPOSE: Finasteride is a competitive inhibitor of 5-alpha reductase type 2 enzyme that is commonly used to treat benign prostatic hyperplasia and male pattern hair loss. It is not clear about the synergistic effects of finasteride and resistance training on protein homeostasis in androgen-target tissue such as skeletal muscle. Thus, the purpose of this study was to investigate the effects of 8-week finasteride and resistance exercise training on protein synthesis and autophagic degradation in rat skeletal muscle.
      METHODS: Forty-eight male wild-type Sprague Dawley rats (8weeks old) were randomly assigned into 4 groups: (1) sedentary control, (2) finasteride, (3) exercise, and (4) exercise plus finasteride. Rats of the finasteride group received finasteride, dissolved in corn oil (10 mg/kg) by oral gavage. Rats of the exercise group climbed a 1-m ladder inclined at 85° every 3 days for 8 weeks as a means of resistance exercise. They climbed the ladder 8 times with the load of 50%, 75%, 90%, and 100% of its body weight. Rates of the exercise plus finasteride group were given both interventions. We assessed autophagy flux, protein synthesis (mTOR signaling and translation rate using the SUnSET assay), and muscular functions before and after 8-weeks of intervention, and performed one-way ANOVA to determine pre-post differences in each group.
      RESULTS: The finasteride treatment significantly reduced protein synthesis while activating autophagic degradation in skeletal muscle of rats. The exercise training increased both protein synthesis and autophagic degradation. The combined treatments decreased both protein synthesis and autophagy flux in the skeletal muscle (p<0.05).
      CONCLUSIONS: Eight weeks of finasteride treatment appears to disturb the protein homeostasis, which is viewed as a balance of protein synthesis and degradation through the reduction in protein synthesis and activation in autophagic degradation simultaneously in skeletal muscle. Resistance exercise appears to alleviate the disruption of protein homeostasis induced by finasteride treatment.

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      참고문헌 (Reference)

      1 Lee S, "Viral expression of insulinlike growth factor-1 enhances muscle hypertrophy in resistancetrained rats" 96 : 1097-1104, 2001

      2 McConnell JD, "The effect of finasteride on the risk of acute urinary retention and the need for surgical treatment among men with benign prostatic hyperplasia. Finasteride Long-Term Efficacy and Safety Study Group" 338 : 557-563, 1998

      3 "The Merck Index" Merck Rehway 2000

      4 Guyton AC, "Textbook of Medical Physiology" W. B 1981

      5 Eslahi A, "Stereological comparison of intraprostatic injection of alcohol and bleomycin with finasteride gavages in rats" 70 (70): 163-169, 2017

      6 Breen L, "Skeletal muscle protein metabolism in the elderly:Interventions to counteract the ‘anabolic resistance’ of aging" 8 : 68-, 2011

      7 Welk B, "Risk of rhabdomyolysis from 5-α reductase inhibitors" 27 (27): 351-355, 2018

      8 Haan J, "Reversible severe myopathy during treatment with finasteride" 20 (20): 502-504, 1997

      9 Ryu HJ, "Reversible myopathy and ophthalmoparesis after low-dose finasteride administration for androgenic alopecia" 40 : 595-597, 2014

      10 Van Rij S, "Recent advances in treatment for Benign Prostatic Hyperplasia" (4) : 2015

      1 Lee S, "Viral expression of insulinlike growth factor-1 enhances muscle hypertrophy in resistancetrained rats" 96 : 1097-1104, 2001

      2 McConnell JD, "The effect of finasteride on the risk of acute urinary retention and the need for surgical treatment among men with benign prostatic hyperplasia. Finasteride Long-Term Efficacy and Safety Study Group" 338 : 557-563, 1998

      3 "The Merck Index" Merck Rehway 2000

      4 Guyton AC, "Textbook of Medical Physiology" W. B 1981

      5 Eslahi A, "Stereological comparison of intraprostatic injection of alcohol and bleomycin with finasteride gavages in rats" 70 (70): 163-169, 2017

      6 Breen L, "Skeletal muscle protein metabolism in the elderly:Interventions to counteract the ‘anabolic resistance’ of aging" 8 : 68-, 2011

      7 Welk B, "Risk of rhabdomyolysis from 5-α reductase inhibitors" 27 (27): 351-355, 2018

      8 Haan J, "Reversible severe myopathy during treatment with finasteride" 20 (20): 502-504, 1997

      9 Ryu HJ, "Reversible myopathy and ophthalmoparesis after low-dose finasteride administration for androgenic alopecia" 40 : 595-597, 2014

      10 Van Rij S, "Recent advances in treatment for Benign Prostatic Hyperplasia" (4) : 2015

      11 Ju JS, "Quantitation of"autophagic flux"in mature skeletal muscle" 6 (6): 929-935, 2010

      12 Grumati P, "Physical exercise stimulates autophagy in normal skeletal muscles but is detrimental for collagen VI-deficient muscles" 7 : 1415-1423, 2011

      13 Goodman CA, "Novel insights into the regulation of skeletal muscle protein synthesis as revealed by a new nonradioactive in vivo technique" 25 : 1028-1039, 2011

      14 Al-harbi TM, "Finasteride-induced myalgia and hyperCKemia" 10 (10): 76-78, 2008

      15 Yu Seob Shin, "Finasteride and Erectile Dysfunction in Patients with Benign Prostatic Hyperplasia or Male Androgenetic Alopecia" 대한남성과학회 37 (37): 157-165, 2019

      16 Ho CK, "Estrongen and androgen signaling in the pathogenesis of BPH" 8 (8): 29-41, 2011

      17 Bhasin S, "Effect of testosterone supplementation with and without a dual 5α-reductase inhibitor on fat-free mass in men with suppressed testosterone production" 37 (37): 931-939, 2012

      18 Bartsch G, "Dihydrotestosterone and the concept of 5 alpha-reductase inhibition in human benign prostatic hyperplasia" 19 : 413-425, 2009

      19 Leedahl DD, "Benign prostatic hyper plasia : implications for pharmacologic treatment and perioperative care" 26 (26): 52-58, 2013

      20 Ju JS, "Autophagy plays a role in skeletal muscle mitochondrial biogenesis in an endurance exercisetrained condition" 66 : 417-430, 2016

      21 Lira VA, "Autophagy is required for exercise training-induced skeletal muscle adaptation and improvement of physical performance" 27 : 4184-4193, 2013

      22 Aartsma-Rus A, "Assessing functional performance in the Mdx mouse model" 85 : e51303-, 2014

      23 Ratamess NA, "Androgen receptor content following heavy resistance exercise in men" 93 (93): 35-42, 2005

      24 "ACSM’s Guidelines for Exercise Training and Prescription" Baltimore Williams & Wilkins 159-, 1995

      25 Naslund MJ, "A review of the clinical efficacy and safety of 5alpha-reductase inhibitors for the enlarged prostate" 29 : 17-25, 2007

      26 Escrich R, "A high-cornoil diet strongly stimulates mammary carcinogenesis, while a high-extra-virgin-olive-oil diet has a weak effect, through changes in metabolism, immune system function and proliferation/apoptosis pathway" 64 : 218-227, 2019

      27 Upreti R, "5α-reductase type 1 modulates insulin sensitivity in men" 969 (969): E1397-E1406, 2014

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      학술지 이력

      학술지 이력
      연월일 이력구분 이력상세 등재구분
      2026 평가예정 재인증평가 신청대상 (재인증)
      2020-01-01 평가 등재학술지 유지 (재인증) KCI등재
      2017-01-01 평가 등재학술지 유지 (계속평가) KCI등재
      2013-01-01 평가 등재 1차 FAIL (등재유지) KCI등재
      2010-01-01 평가 등재학술지 유지 (등재유지) KCI등재
      2008-01-01 평가 등재학술지 유지 (등재유지) KCI등재
      2006-01-01 평가 등재학술지 유지 (등재유지) KCI등재
      2005-03-21 학회명변경 한글명 : 한국운동과학회 -> 한국운동생리학회
      영문명 : Korea Exercise Science Academy -> Korean Society of Exercise Physiology
      KCI등재
      2005-03-21 학회명변경 한글명 : 한국운동과학회 -> 한국운동생리학회
      영문명 : Korea Exercise Science Academy -> Korean Society of Exercise Physiology
      KCI등재
      2003-01-01 평가 등재학술지 선정 (등재후보2차) KCI등재
      2002-01-01 평가 등재후보 1차 PASS (등재후보1차) KCI등재후보
      2001-07-01 평가 등재후보학술지 선정 (신규평가) KCI등재후보
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      학술지 인용정보

      학술지 인용정보
      기준연도 WOS-KCI 통합IF(2년) KCIF(2년) KCIF(3년)
      2016 0.76 0.76 0.67
      KCIF(4년) KCIF(5년) 중심성지수(3년) 즉시성지수
      0.62 0.71 0.674 0.03
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