Protective effect of d-alanine against acute kidney injury

Yasunori Iwata; Yusuke Nakade; Shinji Kitajima; Shiori Yoneda-Nakagawa; Megumi Oshima; Norihiko Sakai; Hisayuki Ogura; Koichi Sato; Tadashi Toyama; Yuta Yamamura; Taro Miyagawa; Hiroka Yamazaki; Akinori Hara; Miho Shimizu; Kengo Furuichi; Masashi Mita; Kenji Hamase; Tomohiro Tanaka; Motohiro Nishida; Wataru Muramatsu; Hisashi Yamamoto; Shigeyuki Shichino; Satoshi Ueha; Kouji Matsushima; Takashi Wada

doi:10.1152/ajprenal.00198.2021

Protective effect of d-alanine against acute kidney injury

Am J Physiol Renal Physiol. 2022 Jun 1;322(6):F667-F679. doi: 10.1152/ajprenal.00198.2021. Epub 2022 Apr 18.

Authors

Yasunori Iwata^{1

2}, Yusuke Nakade², Shinji Kitajima^{3

2}, Shiori Yoneda-Nakagawa², Megumi Oshima², Norihiko Sakai^{3

2}, Hisayuki Ogura², Koichi Sato², Tadashi Toyama², Yuta Yamamura², Taro Miyagawa², Hiroka Yamazaki², Akinori Hara², Miho Shimizu², Kengo Furuichi⁴, Masashi Mita⁵, Kenji Hamase⁶, Tomohiro Tanaka⁷, Motohiro Nishida^{6

7}, Wataru Muramatsu⁸, Hisashi Yamamoto⁸, Shigeyuki Shichino⁹, Satoshi Ueha⁹, Kouji Matsushima⁹, Takashi Wada²

Affiliations

¹ Division of Infection Control, Kanazawa University Hospital, Kanazawa, Japan.
² Department of Nephrology and Laboratory Medicine, Kanazawa University, Kanazawa, Japan.
³ Division of Blood Purification, Kanazawa University Hospital, Kanazawa, Japan.
⁴ Division of Nephrology, Kanazawa Medical University School of Medicine, Kanazawa, Japan.
⁵ KAGAMI Incorporated, Osaka, Japan.
⁶ Graduate School of Pharmaceutical Sciences, Kyushu University, Fukuoka, Japan.
⁷ National Institute for Physiological Sciences and Exploratory Research Center on Life and Living Systems and Center for Novel Science Initiatives, National Institutes of Natural Sciences, Aichi, Japan.
⁸ Molecular Catalyst Research Center, Chubu University, Aichi, Japan.
⁹ Division of Molecular Regulation of Inflammatory and Immune Diseases, Research Institute of Biomedical Sciences, Chiba; Tokyo University of Science, Tokyo, Japan.

PMID: 35435002
DOI: 10.1152/ajprenal.00198.2021

Abstract

Recent studies have revealed the connection between amino acid chirality and diseases. We have previously reported that the gut microbiota produces various d-amino acids in a murine acute kidney injury (AKI) model. Here, we further explored the pathophysiological role of d-alanine (d-Ala) in AKI. Levels of d-Ala were evaluated in a murine AKI model. We analyzed transcripts of the N-methyl-d-aspartate (NMDA) receptor, a receptor for d-Ala, in tubular epithelial cells (TECs). The therapeutic effect of d-Ala was then assessed in vivo and in vitro. Finally, the plasma level of d-Ala was evaluated in patients with AKI. The Grin genes encoding NMDA receptor subtypes were expressed in TECs. Hypoxic conditions change the gene expression of Grin1, Grin2A, and Grin2B. d-Ala protected TECs from hypoxia-related cell injury and induced proliferation after hypoxia. These protective effects are associated with the chirality of d-Ala. d-Ala inhibits reactive oxygen species (ROS) production and improves mitochondrial membrane potential, through NMDA receptor signaling. The ratio of d-Ala to l-Ala was increased in feces, plasma, and urine after the induction of ischemia-reperfusion (I/R). Moreover, Enterobacteriaceae, such as Escherichia coli and Klebsiella oxytoca, produce d-Ala. Oral administration of d-Ala ameliorated kidney injury after the induction of I/R in mice. Deficiency of NMDA subunit NR1 in tubular cells worsened kidney damage in AKI. In addition, the plasma level of d-Ala was increased and reflected the level of renal function in patients with AKI. In conclusion, d-Ala has protective effects on I/R-induced kidney injury. Moreover, the plasma level of d-Ala reflects the estimated glomerular filtration rate in patients with AKI. d-Ala could be a promising therapeutic target and potential biomarker for AKI.NEW & NOTEWORTHY d-Alanine has protective effects on I/R-induced kidney injury. d-Ala inhibits ROS production and improves mitochondrial membrane potential, resulting in reduced TEC necrosis by hypoxic stimulation. The administration of d-Ala protects the tubules from I/R injury in mice. Moreover, the plasma level of d-Ala is conversely associated with eGFR in patients with AKI. Our data suggest that d-Ala is an appealing therapeutic target and a potential biomarker for AKI.

Keywords: acute kidney injury; d-alanine; mitochondria.

MeSH terms

Acute Kidney Injury* / metabolism
Alanine* / therapeutic use
Animals
Apoptosis / genetics
Biomarkers
Humans
Hypoxia
Ischemia
Mice
N-Methylaspartate
Reactive Oxygen Species / metabolism
Receptors, N-Methyl-D-Aspartate
Reperfusion Injury* / metabolism

Substances

Biomarkers
Reactive Oxygen Species
Receptors, N-Methyl-D-Aspartate
N-Methylaspartate
Alanine