Secreted and Transmembrane αKlotho Isoforms Have Different Spatio-Temporal Profiles in the Brain During Aging and Alzheimer's Disease Progression

Overview

Journal PLoS One

Specialties General Medicine
Science

Date 2015 Nov 25

PMID 26599613

Citations 32

Authors

Anna Masso

Angela Sanchez

Lydia Gimenez-Llort

Jose Miguel Lizcano

Manuel Canete

Belen Garcia

Virginia Torres-Lista

Meritxell Puig

Assumpcio Bosch

Miguel Chillon

Affiliations

Soon will be listed here.

Abstract

The Klotho protein is a β-glucuronidase, and its overexpression is associated with life extension. Its mechanism of action is not fully understood, although it has been recently reported that αKlotho improves synaptic and cognitive functions, and it may also influence a variety of structures and functions during CNS maturation and aging. The αKlotho gene has two transcripts, one encoding a transmembrane isoform (m-KL), and the other a putative secreted isoform (s-KL). Unfortunately, little is known about the secreted αKlotho isoform, since available antibodies cannot discriminate s-KL from the KL1 domain cleaved from the transmembrane isoform. This study shows, for the first time, that the klotho transcript produced by alternative splicing generates a stable protein (70 kDa), and that in contrast to the transmembrane Klotho isoform, it is ten times more abundant in the brain than in the kidney suggesting that the two isoforms may have different functions. We also studied whether klotho expression in the CNS was influenced by aging, Alzheimer's disease (AD), or a healthy lifestyle, such as voluntary moderate continuous exercise. We observed a strong correlation between high expression levels of the two klotho transcripts and the healthy status of the animals. Expression of Klotho in brain areas decayed more rapidly in the 3xTg-AD model of AD than in healthy animals, whilst moderate continuous exercise in adulthood prevents the decline in expression of both klotho transcripts.

Citing Articles

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