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Can resemblance (e.g.
correlations) between sib pairs,
or DZ twins, be modeled as a
function of DNA marker sharing
at a particular chromosomal
location?
Three groups of DZ twins



IBD = 2 (all markers identical by descent)
IBD = 1
IBD = 0
Are the correlations (in e.g. lipid levels)
different for the 3 groups?
A fully informative mating
mother
A
father
B
C
D
Q?
Q?
marker
X
Q?
Sib1
AC
BD
Sib1
AC
BD
Sib1
AC
offspring
IBD = 2
offspring
IBD = 1
offspring
IBD = 0
QTL
Sib2
AC
BD
Sib2
AD
BC
Sib2
BD
distance
Q?
Identity By Descent (IBD) status in siblings. Four parental marker
alleles: A - B and C - D. Two sibs can inherit 0, 1 or 2 alleles IBD.
Sib1
AC AD BC
Sib
2
IBD
AC
AD
BC
BD
2
1
1
0
1
2
0
1
1
0
2
1
BD
0
1
1
2
0 : 1 : 2 = 25% : 50% : 25%
Derivation of IBD probabilities for one marker (with and without
parental genotypes known) was given by Haseman and Elston (1972).
Applications: affected sib-pair method
linkage with quantitative traits
Adult Dutch DZ pairs: distribution of pi-hat (π) at 65 cM
(chromosome 19).
π = IBD/2; all pairs with π <0.25 have been assigned to IBD=0 group;
all pairs with
π > 0.75
to IBD=2 group; others to the IBD=1 group.
2 Harold sample (middelb lft)
STUDY:
40
30
20
10
Std. Dev = .30
Mean = .45
N = 117.00
0
.06
PIHAT65
.19
.31
.44
.56
.69
1.00
.88
.75
.63
.50
.38
.25
.13
0.00
.81
.94
Exercise







Model DZ correlation in LDL as a function of IBD
Test if the correlations are the same
Add data of MZ twins
Test if the correlation in the DZ group with IBD =
2 is the same as the MZ correlation
Repeat for apoB and ln(apoE) levels
Does eliminating subjects who are on lipidlowering medication change the results?
Do cross-correlations (across twins/across traits)
differ as a function of IBD? (trivariate)
Basic script and data (LDL, apoB, apoE)




Correlation estimation in DZ:
BasicCorrelationsDZ(ibd).mx
Information on data: datainfo.doc
Datafiles:
DZ: partionedAdultDutch3.dat
MZ: AdultDutchMZ3.dat
Complete (MZ + DZ + tests) job:
AllCorrelations(ibd).mx
Correlations as a function of IBD
IBD2
IBD1
IBD0
MZ
LDL
0.81
0.49
-0.21
0.78
ApoB
lnApoE
0.64
0.83
0.50
0.55
0.02
0.14
0.79
0.89
Correlations as a function of IBD
chi-squared tests
LDL
apoB
apoE
all DZ equal
21.77
7.98
12.45
DZ(ibd2)=MZ
0.0975
1.53
0.576
(df=2)
(df=1)
Can heritability be modeled as a
function of DNA marker sharing
at a particular chromosomal
location?
DZ twin pairs who are IBD = 2: familial and QTL effects
r =1
E
E
r =1
e
e
F
f
DZ 1
F
Q
Q
q
q
f
DZ 2
DZ twin pairs who are IBD = 1: familial and QTL effects
r =1
E
E
r = 0.5
e
e
F
f
DZ 1
F
Q
Q
q
q
f
DZ 2
DZ twin pairs who are IBD = 0: familial effects
r =1
E
E
e
e
F
f
DZ 1
F
f
DZ 2
Linkage analysis in DZ twins
or sib pairs
3 groups: IBD=2,1,0 (π=1, 0.5, 0)
Model the covariance as a function of IBD
Allow for background familial variance
Total variance also includes E
Covariance = πQ + F + E
Variance = Q + F + E
MZ Twin pairs
rMZ = 1
rMZ = 1
E
e
E
rMZ = 1
C
c
C
A
a
MZ 1
A
Q
Q
q
q
a
MZ 2
c
e
rMZ = rDZ = 1
rMZ = 1, rDZ = 0.5
E
e
E
rMZ = 1, rDZ = 0,
0.5 or 1
C
c
C
A
a
Twin 1
A
Q
Q
q
q
e
c
a
Twin 2
4 group linkage analysis (3 IBD DZ groups and 1 MZ group)
Exercise




Fit FQE model to DZ data (i.e. F=familial,
Q=QTL effect, E=unique environment)
Fit FE model to DZ lipid data (drop Q)
Is the QTL effect significant?
Add MZ data: ACQE model (A= additive
genetic effects, C=common environment),
does this change the estimate /
significance of QTL?
Basic script and data (LDL, apoB, apoE)




FQE model in DZ twins: FQEmodel-DZ.mx
Information on data: datainfo.doc
Datafiles:
DZ: partionedAdultDutch3.dat
MZ: AdultDutchMZ3.dat
Complete (MZ data + DZ data + tests) job:
ACEQ-mzdz.mx
Test of the QTL: chi-squared test
(df = 1)
LDL
apoB
apoE
DZ pairs
12.247
1.945
12.448
DZ+MZ pairs
12.561
2.128
12.292
Use pi-hat: single group analysis (DZ only)
rDZ = 0.5
E
E
rDZ = ^
e
e
A
a
Twin 1
A
Q
Q
q
q
a
Twin 2
Exercise: PiHatModelDZ.mx

Chi-square (LDL) = 12.318
rMZ = rDZ = 1
rMZ = 1, rDZ = 0.5
E
e
E
^
rMZ = 1, rDZ = 
C
c
C
A
a
Twin 1
A
Q
Q
q
q
a
Twin 2
c
e
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