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  3. Clinical Laboratory Sciences and Medical Biotechnology / 醫學檢驗暨生物技術學系所
  4. Genetic variations of CD36 and low platelet CD36 expression - a risk factor for lipemic plasma donation in Taiwanese apheresis donors
 
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Genetic variations of CD36 and low platelet CD36 expression - a risk factor for lipemic plasma donation in Taiwanese apheresis donors

Journal
Vox Sanguinis
Journal Volume
110
Journal Issue
3
Pages
236-243
Date Issued
2016
Author(s)
SHYH-CHYI LO  
Lin K.-H.
Hsieh H.-H.
Lin D.-T.
CHUNG-YI HU  
DOI
10.1111/vox.12356
URI
https://scholars.lib.ntu.edu.tw/handle/123456789/552716
Abstract
Background: New CD36 mutations are constantly being identified, although no study has specifically targeted a Taiwanese population. CD36 deficiency can result in dyslipid state and slow clearance of chylomicron. This could be linked to more frequent lipemic donations. Study Design and Methods: We used flow cytometric methods to study the CD36 deficiency in 640 regular volunteer platelet apheresis donors from Taipei blood centre. The coding exons of CD36 gene were sequenced in CD36-deficient individuals, and the allele frequencies of CD36 variants were determined in the larger population by mutation-specific PCR and oligonucleotide hybridization. Visual inspection of lipemic plasma was routinely performed on samples taken before commencement of apheresis. Individuals found to have lipemic plasma are deferred until next donation. We investigated the link between positive lipemic deferral record and low platelet CD36 expression status. Results: We found four donors (0·6%) with type I CD36 deficiency (both platelets and monocytes CD36null) and six (1·0%) with type II CD36 deficiency (PLT: CD36null, monocyte: CD36low). Six CD36 genetic variants were identified, two of them were novel, all but one are found exclusively in CD36null and CD36low expressors. Subjects with CD36 genetic variants also displayed deficient or reduced CD36 on monocytes. Donors with null or low PLT CD36 expression were more likely to have a lipemic deferral record than control subjects with normal PLT CD36 expression (X2 = 27·36, odds ratio = 2·6, 95% conference interval: 1·8-3·8, P < 0·0001). Conclusion: Through this study, we established a donor registry to supply CD36-negative platelets for patients in need. ? 2016 International Society of Blood Transfusion.
SDGs

[SDGs]SDG3

Other Subjects
CD36 antigen; thrombocyte antigen; CD36 antigen; lipid; antigen expression; apheresis; Article; blood donor; CD36 deficiency; clinical article; controlled study; correlation analysis; exon; female; flow cytometry; gene frequency; gene mutation; gene sequence; genetic variability; heterozygote; human; human cell; hybridization; hyperlipidemia; male; monocyte; polymerase chain reaction; prevalence; priority journal; protein deficiency; register; risk factor; sequence specific oligonucleotide probe hybridization; Taiwanese; thrombocyte; Asian continental ancestry group; blood; blood donor; Blood Platelet Disorders; Genetic Diseases, Inborn; genetic polymorphism; genetics; metabolism; pathology; Taiwan; thrombocytopheresis; Antigens, CD36; Asian Continental Ancestry Group; Blood Donors; Blood Platelet Disorders; Blood Platelets; Exons; Female; Flow Cytometry; Gene Frequency; Genetic Diseases, Inborn; Humans; Lipids; Male; Monocytes; Plateletpheresis; Polymerase Chain Reaction; Polymorphism, Genetic; Risk Factors; Taiwan
Type
journal article

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