Journal
PLOS ONE
Volume 17, Issue 5, Pages -Publisher
PUBLIC LIBRARY SCIENCE
DOI: 10.1371/journal.pone.0267298
Keywords
-
Categories
Funding
- National Institutes of Health [R01AG044546, P01AG003991, RF1AG053303, R01AG058501, U01AG058922, RF1AG058501, R01AG057777]
- Alzheimer Association [NIRG-11-200110, BAND-14-338165, AARG-16-441560, BFG-15-362540]
- Hope Center for Neurological Disorders
- Department of Neurology at Washington University School of Medicine
- NIH [P50 AG05681, P01 AG03991, P01 AG026276]
- Swedish Research Council [2017-00915, 201809-2016862]
- European Research Council [681712]
- Swedish State Support for Clinical Research [ALFGBG-720931]
- Alzheimer Drug Discovery Foundation (ADDF), USA [RDAPB-201809-2016615, FO2019-0228]
- Department of Psychiatry at Washington University School of Medicine [ADSF-21-831376-C, ADSF-21-831381-C, ADSF-21-831377-C]
- AD Strategic Fund
- The County Councils, the ALF-agreement [ADSF-21-831381-C, ADSF-21-831377-C, FO2017-0243]
- Alzheimer's Association
- Olav Thon Foundation
- Erling-Persson Family Foundation
- Stiftelsen for Gamla Tjanarinnor
- Hjarnfonden, Sweden [860197, ALFGBG-715986]
- European Union [AF-742881]
- UK Dementia Research Institute at UCL
- Swedish Alzheimer Foundation [ALFGBG-715986]
- Swedish government [JPND2019-466-236]
- European Union Joint Program for Neurodegenerative Disorders [1R01AG068398-01]
- National Institute of Health (NIH), USA [ZEN-21-848495]
- Alzheimer's Association 2021 Zenith Award [2018-02532]
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Two genetic variants in the KL gene are associated with Alzheimer's disease risk and may lower the incidence of neurodegeneration and cognitive decline.
Two genetic variants in strong linkage disequilibrium (rs9536314 and rs9527025) in the Klotho (KL) gene, encoding a transmembrane protein, implicated in longevity and associated with brain resilience during normal aging, were recently shown to be associated with Alzheimer disease (AD) risk in cognitively normal participants who are APOE epsilon 4 carriers. Specifically, the participants heterozygous for this variant (KL-SVHET+) showed lower risk of developing AD. Furthermore, a neuroprotective effect of KL-VSHET+ has been suggested against amyloid burden for cognitively normal participants, potentially mediated via the regulation of redox pathways. However, inconsistent associations and a smaller sample size of existing studies pose significant hurdles in drawing definitive conclusions. Here, we performed a well-powered association analysis between KL-VSHET+ and five different AD endophenotypes; brain amyloidosis measured by positron emission tomography (PET) scans (n = 5,541) or cerebrospinal fluid A beta 42 levels (CSF; n = 5,093), as well as biomarkers associated with tau pathology: the CSF Tau (n = 5,127), phosphorylated Tau (pTau181; n = 4,778) and inflammation: CSF soluble triggering receptor expressed on myeloid cells 2 (sTREM2; n = 2,123) levels. Our results found nominally significant associations of KL-VSHET+ status with biomarkers for brain amyloidosis (e.g., CSF A beta positivity; odds ratio [OR] = 0.67 [95% CI, 0.55-0.78], beta = 0.72, p = 0.007) and tau pathology (e.g., biomarker positivity for CSF Tau; OR = 0.39 [95% CI, 0.19-0.77], beta = -0.94, p = 0.007, and pTau; OR = 0.50 [95% CI, 0.27-0.96], beta = -0.68, p = 0.04) in cognitively normal participants, 60-80 years old, who are APOE e4-carriers. Our work supports previous findings, suggesting that the KL-VSHET+ on an APOE epsilon 4 genotype background may modulate A beta and tau pathology, thereby lowering the intensity of neurodegeneration and incidence of cognitive decline in older controls susceptible to AD.
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