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NRF2 pathway activation attenuates ageing-related renal phenotypes due to α-klotho deficiency

Mingyue Zhao, Shohei Murakami, Daisuke Matsumaru, Takeshi Kawauchi, Yo‐ichi Nabeshima, Hozumi Motohashi

2022The Journal of Biochemistry21 citationsDOI

Abstract

Oxidative stress is one of the major causes of the age-related functional decline in cells and tissues. The KEAP1-NRF2 system plays a central role in the regulation of redox balance, and NRF2 activation exerts antiageing effects by controlling oxidative stress in aged tissues. α-Klotho was identified as an ageing suppressor protein based on the premature ageing phenotypes of its mutant mice, and its expression is known to gradually decrease during ageing. Because α-klotho has been shown to possess antioxidant function, ageing-related phenotypes of α-klotho mutant mice seem to be attributable to increased oxidative stress at least in part. To examine whether NRF2 activation antagonizes ageing-related phenotypes caused by α-klotho deficiency, we crossed α-klotho-deficient (Kl-/-) mice with a Keap1-knockdown background, in which the NRF2 pathway is constitutively activated in the whole body. NRF2 pathway activation in Kl-/- mice extended the lifespan and dramatically improved ageing-related renal phenotypes. With elevated expression of antioxidant genes accompanied by an oxidative stress decrease, the antioxidant effects of NRF2 seem to make a major contribution to the attenuation of ageing-related renal phenotypes of Kl-/- mice. Thus, NRF2 is expected to exert an antiageing function by partly compensating for the functional decline of α-Klotho during physiological ageing.

Topics & Concepts

KlothoAgeingOxidative stressPhenotypeKEAP1Cell biologyGene knockdownBiologyOxidative phosphorylationAntioxidantEndocrinologyInternal medicineKidneyMedicineGeneticsBiochemistryGeneTranscription factorParathyroid Disorders and TreatmentsHeterotopic Ossification and Related ConditionsKruppel-like factors research
NRF2 pathway activation attenuates ageing-related renal phenotypes due to α-klotho deficiency | Litcius