Serum progranulin is not associated with rs5848 polymorphism in Korean patients with neurodegenerative diseases

Author:

Jung Na-YeonORCID,Kim Hyang-Sook,Kim Eun Soo,Jeon Sumin,Lee Myung Jun,Pak Kyoungjune,Lee Jae-Hyeok,Lee Young Min,Lee Kangyoon,Shin Jin-Hong,Ko Jun Kyeung,Lee Jae Meen,Yoon Jin A.,Hwang Chungsu,Choi Kyung-Un,Huh Gi Yeong,Kim Young-Eun,Kim Eun-Joo

Abstract

Low serum progranulin (PGRN) is known to be associated with granulin (GRN) gene mutation and T alleles ofGRNrs5848 polymorphism. However, there have been only a few Asian studies exploring these. We investigated the serum PGRN levels, rs5848 genotypes, and their relations with cerebrospinal fluid (CSF) Alzheimer’s disease (AD) biomarkers in the Korean population. Serum PGRN levels,GRNrs5848 polymorphism, andGRNmutations were evaluated in 239 participants (22 cognitively unimpaired participants and 217 patients with neurodegenerative diseases). CSF AD biomarkers were also evaluated in 214 participants. There was no significant difference in the serum PGRN levels among the diagnostic groups. We could not find anyGRNmutation carrier in our sample. The differences in the frequencies of the rs5848 genotypes among the clinical groups or the effects of the rs5848 genotypes on serum PGRN were not observed. There was no correlation between the serum PGRN level or rs5848 genotype and CSF AD biomarkers. Neither the T allele nor the TT genotype had an effect on the development of AD. Our results showed that serum PGRN levels were not associated with rs5848 genotypes, indicating that multiple single nucleotide polymorphisms might affect PGRN concentrations in an ethnicity-specific manner.

Funder

Korea Centers for Disease Control and Prevention

Ministry of Education

Ministry of Health and Welfare

Publisher

Public Library of Science (PLoS)

Subject

Multidisciplinary

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