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Lipid Metabolizing Genes

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Title: Lipid Metabolizing Genes

1
Lipid Metabolizing Genes
2
Cholesterol Metabolism

CETP
Cholesterol ester transfer protein
Closely linked to HDL-C
HDL-C functions in reverse cholesterol transport
Removes excess cholesterol from periphery
Excess cholesterol is esterified to make
cholesterol esters
CETP and HDL-C
Cholesterol esters may be transferred from HDL-C
to LDL-C
Performed by CETP

3
CETP

Overactive CETP transfers more cholesterol from
HDL-C to LDL-C
Underactive CETP results in more cholesterol
remaining with HDL-C
CETP Inhibitors (Stein Stein, Athersclerosis
2005)
Increase HDL-C
Reduce CVD risk

4
CETP and genetic variants
16/Ex14
9/3
383/In8
VNTR-1946
-629/Prom
82/Ex15
199/In12
279/In1
1
2
3 4 5
11
12 13 14
15 16
6 7 8
9
10
Taq1B
MspI
I405V
R451Q
Thompson et al. 2003 Atherosclerosis
5
CETP 279 G?A

Commonly referred to as Taq1B SNP
Associated with lower CETP mass and higher HDL
Intronic SNP
No obvious link to functional activity
Linked to another common SNP?
Linked SNP tend to be inherited together
Linkage Disequilibrium

6
Linkage Disequilibrium

SNPs are often inherited together and travel as
blocks from generation to generation, this is
known as linkage disequilibrium (Duff 2006, AJCN)
Linkage disequilibrium can be described as the
inheritance of same chromosome SNPs together at a
frequency greater than chance.
Occurs when genotype frequencies at one locus are
dependent on genotype frequencies at the second
(locushttp//www.evotutor.org/EvoGen/EG4A.html)
Can arise from physical linkage, genetic drift
and selection on multilocus genotypes
Two loci are in linkage equilibrium if genotype
frequencies at one locus are independent of
genotype frequencies at the second locus
(locushttp//www.evotutor.org/EvoGen/EG4A.html)

7
Haplotypehttp//www.genome.gov/10001665

Groups of co-inherited SNPs on the same
chromosome (Duff 2006, AJCN)
There could be many haplotypes in a chromosome
region
Recent studies are finding only a few common
haplotypes.
For CETP
CETP 279G?A is closely linked to -629C?A (Klerkx
et al 2003 Human molecular genetics)
Four possible haplotypes for these 2 SNPs
GC, GA, AC, AA
Likely only two are common
GC (normal), AA (variant)

8
Haplotype Example 1

Region with 6 SNPs
DNA bases that are same are not shown
First SNP has alleles A and G
Second SNP has alleles C and T
4 possible haplotypes for these 2 SNPs
AC, AT, GC, GT
Only AC and GT are common
These SNPs are said to be highly associated with
each other (ie, in linkage disequilibrium)

9
Haplotype Example 2

If a region has only a few haplotypes
Only a few SNPs need to be typed to determine
which haplotype a chromosome has
Example below
Determine SNP 1 and 4 and will know haplotype
Saves time and money

10
CETP and Haplotype
Knoblauch et al. 2002
11
Knoblauch et al. 2002
12
Examination of haplotype yields a more
significant effect than examination of SNPs
individually.
13
123456
1 2 3 4 5 6
A/C
G/A
Linkage Disequilibrium 279 A allele is
always inherited with the -629 C allele. A
allele is a marker only (not a functional SNP)
14
Lipid Metabolizing Genes
15
LPL (Lipoprotein Lipase)

Hydrolyzes triglycerides of chylomicrons (CM) and
VLDL

TG degradative products
CM
CM Remnant
Liver
Intestine
LPL
TG degradative products
Liver
LDL
Tissues
VLDL
LPL
16
LPL Activity

Positive relationship with HDL-C
gt LPL activity gt serum HDL-C
Via contributing surface components to HDLC
Negative relationship with TGs
gtLPL activity lt serum TGs

17
LPL GeneKnoblauch et al. 2002, Human Molecular
Genetics
LPL 1595 C?G
Cytogenic Location 8p22
18
LPL C1595G

More commonly referred to as the 447 Serine?Stop
substitution (S447X)
Located in exon 9
Produces a truncated protein lacking two amino
acids (serine-glycine) at the carboxy terminus
Appears to be a functional polymorphism

19
X447 allele (LPL 1595 G allele)

Associated with
Increased enzyme activity
Lower serum TGs
Higher serum HDL-C
Reduced risk of CAD (OR 0.4)
Frequency is higher in Caucasians than African
Americans

(Chen et al. 2001 Atherosclerosis)
20
HDL-C and TGs in carriers and non-carriers of the
LPL 1595 G allele
Plt0.01
Plt0.05
Combined data from adult Causasian and African
American men and women
(Chen et al. 2001 Atherosclerosis)
21
Lipid Metabolizing Genes
22
Apolipoprotein CIII (ApoC-III)

Located on Chromosome 11
11p21 (short arm)
Mainly synthesized in liver
Lesser degree in intestine
Component of TG rich lipoproteins (VLDL and CMs)
and HDL
Function is poorly understood

23
Proposed Function(s)

Triglyceride Metabolism
Invitro Studies
Non-competitive inhibitor of LPL
Reduced VLDL and CM catabolism
Mice studies
Overexpression of human apo C-III resulted in
marked hypertriglyceridemia
Humans
Elevated apoC-III levels are associated with
hypertriglyceridemia

24
ApoC-III 3175 C?G

Exon 4 of Chromosome 11p21
Variant is transcribed but not translated
Does not change protein sequence
May be linked to another variant that alters
(increases) Apo C3 expression
Commonly referred to as SstI
Identified with SstI (restriction enzyme)
May also include variants at -641, -482, -455,
1100
Group is often referred to as Sst1 S1/S2 site
(Tobin et al. 2004)
Linked to elevated triglycerides
Associated with premature heart disease in some
studies

25
ApoC-III 3175 C?G and TGs in controls

Additional Comments
Frequency of G allele
tended (P0.06) to be
higher in cases with CVD
More studies are needed to
determine how a mutation at
this site may be linked to other
mutations that affect protein
function.

Ordovas et al. 1991 Atherosclerosis
26
ApoC3 and Haplotype and CVD riskC(-641)A,
C(-482)T, T(-455)C, C1100T, C3175G, T3206G
Tobin et al. 2004 European Heart Journal
27
Lipid Metabolizing Genes
28
Personalized Dietary Recommendations