4.7 Article

Detrimental Effects of Chronic L-Arginine Rich Food on Aging Kidney

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FRONTIERS IN PHARMACOLOGY
卷 11, 期 -, 页码 -

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FRONTIERS MEDIA SA
DOI: 10.3389/fphar.2020.582155

关键词

aging; arginase; kidney; arginine supplementation; inflammation

资金

  1. Swiss National Science Foundation [31003A_159582/1, 31003A_179261/1]
  2. Swiss Heart Foundation [FF19033]
  3. National Centre of Competence in Research Program (NCCR-Kidney.CH)
  4. Swiss National Science Foundation (SNF) [31003A_179261] Funding Source: Swiss National Science Foundation (SNF)

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The study found that long-term L-arginine supplementation has negative effects on kidney aging, leading to increased inflammation and fibrosis markers, enhanced albuminuria, and mortality particularly in females.
The impaired L-arginine/nitric oxide pathway is a well-recognized mechanism for cardiovascular and renal diseases with aging. Therefore, supplementation of L-arginine is widely proposed to boost health or as adjunct therapy for the patients. However, clinical data, show adverse effects and even enhanced mortality in patients receiving long-term L-arginine supplementation. The effects of long-term L-arginine supplementation on kidney aging and the underlying mechanisms remain elusive. Moreover, high protein and high amino acid diet has been thought detrimental for kidney. We therefore investigated effects of chronic dietary L-arginine supplementation on kidney aging. In both young (4 months) and old (18-24 months) mice, animals either receive standard chow containing 0.65% L-arginine or diet supplemented with L-arginine to 2.46% for 16 weeks. Inflammation and fibrosis markers and albuminuria are then analyzed. Age-associated increases in tnf-alpha, il-1 beta, and il-6, vcam-1, icam-1, mcp1, inos, and macrophage infiltration, collagen expression, and S6K1 activation are observed, which is not favorably affected, but rather further enhanced, by L-arginine supplementation. Importantly, L-arginine supplementation further enhances age-associated albuminuria and mortality particularly in females, accompanied by elevated renal arginase-II (Arg-II) levels. The enhanced albuminuria by L-arginine supplementation in aging is not protected in Arg-II-/- mice. In contrast, L-arginine supplementation increases ROS and decreases nitric oxide production in old mouse aortas, which is reduced in Arg-II-/- mice. The results do not support benefits of long-term L-arginine supplementation. It rather accelerates functional decline of kidney and vasculature in aging. Thus, the long-term dietary L-arginine supplementation should be avoided particularly in elderly population.

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