Hyperlipidemia Clinical Trial
Official title:
Studies of Apolipoprotein Genotyping on the Drug Treatment of Hyperlipidemic Patients
Cardiovascular-related diseases have been the majorities of the leading ten causes of death
in Taiwan. Atherosclerotic cardiovascular diseases are multifactorial. Some non-modifiable
risk factors (e.g. genetic trait) may attenuate the benefit of risk modification of the
modifiable factors (e.g. the effect of drug treatment). Genetic epidemiology has being
widely used to analyze the underline risk of cardiovascular diseases and to point the
direction of treatment or prevention.
Lipoprotein is composed of lipid and protein. The genetic variation or mutation of
apolipoprotein, the protein of lipoprotein, has been linked to some lipid abnormality
resulting severe atherosclerotic cardiovascular diseases. ApoA-I, apo A-II, apo A-IV, apo
B100, apo B48, apo C-I, apo C-II, apo C-III, apo D, and apo E are currently thought to
affect lipid abnormalities. In addition, it has been documented that genetic variations are
presented among different races. Apolipoprotein genetic variations or genetic polymorphism
study has been emerged as an important role in the field of genetic therapy. The purpose of
this 3-year study is to continue the lipid study in our laboratory, identifying the
apolipoprotein genotyping in our pooled hyperlipidemic patients and normal control subjects
living in Taiwan. We will observe the incidence and link apo A-I, apo A-II, apo A-IV and apo
C-III genetic variations to the related lipid abnormality and cardiovascular diseases. The
changes of genotyping after lipid lowering drug treatment using statin or fibrate in
hypercholesterolemic or hypertriglyceridemic patients is another goal of this project.
Cardiovascular-related diseases have been the majorities of the leading ten causes of death
in Taiwan. Atherosclerotic cardiovascular diseases are multifactorial. Some non-modifiable
risk factors (e.g. genetic trait) may attenuate the benefit of risk modification of the
modifiable factors (e.g. the effect of drug treatment). Genetic epidemiology has being
widely used to analyze the underline risk of cardiovascular diseases and to point the
direction of treatment or prevention.
Lipoprotein is composed of lipid and protein. The genetic variation or mutation of
apolipoprotein, the protein of lipoprotein, has been linked to some lipid abnormality
resulting severe atherosclerotic cardiovascular diseases. ApoA-I, apo A-II, apo A-IV, apo
B100, apo B48, apo C-I, apo C-II, apo C-III, apo D, and apo E are currently thought to
affect lipid abnormalities. In addition, it has been documented that genetic variations are
presented among different races. Apolipoprotein genetic variations or genetic polymorphism
study has been emerged as an important role in the field of genetic therapy. The purpose of
this 3-year study is to continue the lipid study in our laboratory, identifying the
apolipoprotein genotyping in our pooled hyperlipidemic patients and normal control subjects
living in Taiwan. We will observe the incidence and link apo A-I, apo A-II, apo A-IV and apo
C-III genetic variations to the related lipid abnormality and cardiovascular diseases. The
changes of genotyping after lipid lowering drug treatment using statin or fibrate in
hypercholesterolemic or hypertriglyceridemic patients is another goal of this project.
Our results showed ApoC-III (3175NT C→G) mutation was significantly related to
hypertriglyceridemia, the same relation was also found in the Apo B exon 29 (13132 NT C→G;
4311 AA Asn →Ser) mutation. It is interesting to find some hot spot mutation among Caucasian
population, such as Apo B exon 26 (10699 NT C→A; 3500 AA Arg →Gln), Apo A-IV (1527-2345 NT)
and Apo E exon 2 mutations, were not found in tested samples. Most of presented allele
frequencies in apolipoteins genes were different between our population and Caucasian
population. The present results strongly suggest that it is necessary to establish our own
genetic data which are linked to diseases.
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Observational Model: Case Control, Time Perspective: Cross-Sectional
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