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    208

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    Karla

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    of 3

    PMID- 28623937

    OWN - NLM
    STAT- MEDLINE
    DCOM- 20180403
    LR - 20211204
    IS - 1476-511X (Electronic)
    IS - 1476-511X (Linking)
    VI - 16
    IP - 1
    DP - 2017 Jun 17
    TI - The association of lipid metabolism relative gene polymorphisms and ischemic
    stroke in Han and Uighur population of Xinjiang.
    PG - 120
    LID - 10.1186/s12944-017-0491-9 [doi]
    LID - 120
    AB - BACKGROUND: The present study is aimed to evaluate difference of lipid
    metabolism
    related gene single nucleotide polymorphisms (SNPs) with ischemic stroke (IS)
    in
    Han and Uighur population of Xinjiang, China. METHODS: Four hundred eight
    patients with ischemic stroke and 347 unrelated healthy individuals of age
    and
    sex matched were genotyped for Apolipoprotein A5 (ApoA5), lipoprotein lipase
    (LPL), Cholesteryl ester transfer protein (CETP) and low-density lipoprotein
    receptor (LDL-R) genes. Their mutation difference was analyzed by SNaP shot
    techniques. GeneMapper4.1 SPSS20.0 software was used for data management and
    analysis. Using a single locus analysis, the distribution difference of
    genotype
    loci in ischemic stroke cases and controls were detected to assess the
    genetic
    risk factors of ischemic stroke. RESULTS: Significance differences of
    genotype
    distribution in ischemic stroke cases and controls were observed in LDLR
    rs688 in
    Han and Uighur population in recessive model from analysis of single gene
    locus.
    It also was found that dramatic difference of triglyceride (TG) of LPL rs328
    and
    systolic blood pressure in CETP rs708277 of total population. In binary
    logistic
    regression analysis of total studied population, ischemic stroke was observed
    significantly associated with LDLR rs688 both addictive model (TT/CC,
    adjusted
    OR = 1.47, 95% CI = 1.04-2.07) and recessive model (TT/CT + CC, adjusted Odds
    ratio (OR) = 2.66, 95% Confidence Interval (CI) = 1.37-5.14). In Han
    population,
    ischemic stroke was observed significantly associated with rs688 both in
    addictive model (TT/CC, adjusted OR = 3.27, 95% CI = 1.06-10.05). In Uighur
    population, no significant association was found between gene polymorphisms
    and
    the risk of ischemic stroke. Combined analysis of multiple gene and loci,
    interaction effects of LDLR rs688 C/T, ApoA5 rs662799 A/G and CETP rs708272
    C/T
    denoted a significant influence on IS susceptibility. CONCLUSION: Single
    nucleotide polymorphisms of lipid metabolism relative gene were significantly
    associated with the morbidity of ischemic stroke in Han population. The
    interaction effects of rs688 C/T with ApoA5 rs662799 A/G and CETP rs708272
    C/T
    promoted the occurrence of IS.
    FAU - Yue, Yun-Hua
    AU - Yue YH
    AD - Department of Neurology, Yangpu Hospital Tongji University School of
    Medicine,
    No. 450 Tengyue Road, Shanghai, 200090, China. 447879206@qq.com.
    FAU - Liu, Ling-Yun
    AU - Liu LY
    AD - Department of Neurology, Yangpu Hospital Tongji University School of
    Medicine,
    No. 450 Tengyue Road, Shanghai, 200090, China.
    FAU - Hu, Liang
    AU - Hu L
    AD - Department of Neurology, Yangpu Hospital Tongji University School of
    Medicine,
    No. 450 Tengyue Road, Shanghai, 200090, China.
    FAU - Li, You-Mei
    AU - Li YM
    AD - Department of Neurology, Yangpu Hospital Tongji University School of
    Medicine,
    No. 450 Tengyue Road, Shanghai, 200090, China.
    FAU - Mao, Jie-Ping
    AU - Mao JP
    AD - Department of Neurology, Friendship Hospital to Urumqi, Urumqi, 830049,
    China.
    FAU - Yang, Xiao-Ying
    AU - Yang XY
    AD - Department of Neurology, Friendship Hospital to Urumqi, Urumqi, 830049,
    China.
    FAU - Dila, Na-Mu
    AU - Dila NM
    AD - Department of Neurology, Friendship Hospital to Urumqi, Urumqi, 830049,
    China.
    LA - eng
    PT - Journal Article
    DEP - 20170617
    TA - Lipids Health Dis
    JT - Lipids in health and disease
    JID - 101147696
    RN - 0 (APOA5 protein, human)
    RN - 0 (Apolipoprotein A-V)
    RN - 0 (Cholesterol Ester Transfer Proteins)
    RN - EC 3.1.1.34 (Lipoprotein Lipase)
    SB - IM
    MH - Aged
    MH - Alleles
    MH - Apolipoprotein A-V/genetics/metabolism
    MH - Asians
    MH - Brain Ischemia/genetics/*metabolism
    MH - China
    MH - Cholesterol Ester Transfer Proteins/genetics/metabolism
    MH - Female
    MH - Genetic Predisposition to Disease/genetics
    MH - Genotype
    MH - Humans
    MH - Lipid Metabolism/*genetics/physiology
    MH - Lipoprotein Lipase/genetics/metabolism
    MH - Male
    MH - Middle Aged
    MH - Polymorphism, Single Nucleotide/genetics
    MH - Stroke/genetics/*metabolism
    PMC - PMC5474057
    OTO - NOTNLM
    OT - Apolipoprotein
    OT - Ischemic stroke
    OT - Low density lipoprotein receptor
    OT - Single nucleotide polymorphism
    EDAT- 2017/06/19 06:00
    MHDA- 2018/04/04 06:00
    CRDT- 2017/06/19 06:00
    PHST- 2017/03/15 00:00 [received]
    PHST- 2017/05/22 00:00 [accepted]
    PHST- 2017/06/19 06:00 [entrez]
    PHST- 2017/06/19 06:00 [pubmed]
    PHST- 2018/04/04 06:00 [medline]
    AID - 10.1186/s12944-017-0491-9 [pii]
    AID - 491 [pii]
    AID - 10.1186/s12944-017-0491-9 [doi]
    PST - epublish
    SO - Lipids Health Dis. 2017 Jun 17;16(1):120. doi: 10.1186/s12944-017-0491-9.

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