Meiosis, recombination, and interferencekbroman/presentations/meiosis_nz.pdf · Meiosis: production...
Transcript of Meiosis, recombination, and interferencekbroman/presentations/meiosis_nz.pdf · Meiosis: production...
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Meiosis, recombination,and interference
Karl W Broman
Department of BiostatisticsJohns Hopkins UniversityBaltimore, Maryland, USA
www.biostat.jhsph.edu/˜kbroman
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Outline
� Mitosis and meiosis
� Chiasmata, crossovers
� Genetic distance
� Genetic markers, recombination
� Chromatid and chiasma interference
� Mather’s formula
� The count-location model
� The gamma model and the ��
model
� Data: humans and mice
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Mitosis: ordinary cell division
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Mitosis: ordinary cell division
Chromosomesduplicate
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Mitosis: ordinary cell division
Chromosomesduplicate
Chromosomesline up
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Mitosis: ordinary cell division
Chromosomesduplicate
Chromosomesline up
Chr’s pull apartand cell divides
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Meiosis: production of sex cells
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Meiosis: production of sex cells
Chromosomesduplicate
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Meiosis: production of sex cells
Chromosomesduplicate
Chromosomespair up
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Meiosis: production of sex cells
Chromosomesduplicate
Chromosomespair up
Chr’s exchange materialand cell divides
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Meiosis: production of sex cells
Chromosomesduplicate
Chromosomespair up
Chr’s exchange materialand cell divides
Chr’s pull apartand cells divide
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The exchange process
Vocabulary
Four-strand bundleMeiotic products
Sister chromatidsNon-sister chromatids
Chiasma, chiasmataCrossovers
Obligate chiasma
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Genetic distance
Two points are d Morgans apart if the average number of crossoversper meiotic product in the intervening interval is d .
Usual units: centiMorgan (cM); 100 cM = 1 Morgan
Genetic distance
��� Physical distance
The intensity of the crossover process varies by
� Sex
� Individual
� Chromosome
� Position on chromosome
� Temperature
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But we don’t observe crossovers
Crossoverprocess
Markerdata
� Crossovers generally notobserveable
� We instead observe the originof DNA at marker loci.
odd no. crossovers = recombination event
even no. crossovers = no recombination
Recombination fraction = Pr(recombination event in interval)
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Microsatellite markers
aka Short Tandem Repeat Polymorphisms (STRPs)
G
C
A
T
T
A
A
T
G
C
A
T
T
A
A
T
G
C
A
T
T
A
A
T
� Tandem repeat of something likeGATA at a specific position in thegenome.
� Number of repeats varies
� Use PCR to “amplify” region
� Use gel electrophoresis to determinelength of region
+
−
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Map functions
Connect genetic distance (average no. crossovers)to recombination fraction (chance of an odd no. crossovers).
r � M
�
d
�
d � M-1 �r
�
We require a model for the crossover process.
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Interference
Chromatid interference:
strand choice
Chiasma interference:
positions of chiasmata
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Mather’s formula
Assuming no chromatid interference (NCI):
Pr(no rec’n in interval) = 12
1 – Pr(no chiasma in interval)
� �
[in random meiotic product] [on 4-strand bundle]
Let n = no. chiasmata in interval on 4-strand bundleand m = no. crossovers in interval on random meiotic product
Under NCI, m
�
n Binomial(n, 1/2)
Thus Pr(m is odd�
n) =0 if n = 01/2 if n
�
1
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Haldane map function
Under no interference, the locations of chiasmata on the 4-strandbundle are according to a Poisson process (rate: 2 per Morgan).
Thus n Poisson(2 d)where d is the genetic length of the interval (in Morgans)
Thus Pr(n = 0) = exp(-2 d)
Thus
r = 12
1 – exp(-2 d)
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Models for recombination
chiasmata on4−strand bundle
XOs on randommeiotic product
Thin by 1/2
� Assuming NCI, thin �-process by 1/2, independently,to get the XO-process.
� Models:
– Count-location model– Gamma model, � � model
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Count-location (CL) model
Let n = no. chiasmata on 4-strand bundle
Model: n p = (p0, p1, p2, . . . )
locations
�
n iid uniform(0,L)
Note: p = Poisson(2L) � � no interference
Under NCI, crossovers on random meiotic product will also followa count-location model.
Let m = no. crossovers on random meiotic product
Then m
�
n Binomial(n, 1/2) and
Pr
�
m � i
� � �
n �0 pn
�ni
� �12
�n
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The CL model stinks
Advantage: Can easily incorporate obligate chiasma
Disadvantage: Fits data poorly!
� � Allows crossovers to be too close together.
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Gamma model
Locations of chiasmata according to a stationarygamma renewal process.
Increments are iid gamma(shape = �, rate = 2 �)(Constrained to have mean 1/2 Morgan.)
�
� 1 no interference
� 1 positive chiasma interference
Locations of crossovers on random meiotic product alsoa stationary renewal process.
Inter-arrival distribution is a mixture of gammas
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0 25 50 75 100
Distance (cM)
Inter−chiasma densities
ν12.64.311.350
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0 50 100 150 200
Distance (cM)
Inter−crossover densities
ν12.64.311.350
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Chi-square model
Special case of the gamma model when the parameter is a non-negative integer (take m = � – 1).
Computer simulations and many calculations are easier.
Chiasmata on the 4-strand bundle: take every mth point from aPoisson process with rate 2m per Morgan.
Inter-arrival distribution is a scaled version of a � � distribution.
Example: (m = 4)
0 L
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The gamma model
Advantage: Fits data reasonably well
Disadvantage: Doesn’t account for obligate chiasma
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Human data
� http://research.marshfieldclinic.org/genetics
� 8 CEPH families
– three generations– 11 to 15 progeny– 92 meioses, total
� 8000 STRP markers ( 90% typed)
� Average spacing:
– Female: 0.6
�
1.2 cM– Male: 0.4
�
1.0 cM
� Data cleaning
– Removed 764/954,425 ( 0.08%) genotypes resulting in tightdouble recombinants
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CEPH pedigree(data on 3 markers)
513
525
435
513
224
413
413
427
513
435
224
413
513
424
435
413
435
413
435
224
513
413
513
224
435
213
513
223
513
413
413
413
513
413
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CEPH individual 1331–11maternal chr 10 haplotype
1111111--- 11-111-11- --11--1111 1-11---11-111111--1- 11-1111-11 --11111-11 1111-1111111--111111 111-1111-1 1111111111 10000-0-000--000-000 0000-00000 0000--0000 0000--00000000-00000 000-0--0-- --0-11-11- -1111111-1---1-1-1-1 1111-1--11 11111-1111 -111-11111-1----1111 111111-111 -1111-111- 11-1111111111-11111- 1111111-1- 1111111-11 11-111111-11--1-11-1 111-11-1-1 1-1----1-1 11-111111111--1--11- 11111--111 11--111111 1111-111111-0---0000 00000-0000 00-000
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0 100 200 300 400 500 600
0
200
400
600
800
Raw Data
No. markers between recombinations
0 100 200 300 400 500 600
0
200
400
600
800
Clean Data
No. markers between recombinations
0 5 10 15 20
No. markers between recombinations
0
20
40
60
760
0 5 10 15 20
0
20
40
60
80
100
No. markers between recombinations
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The data
3456789
10111617
0 50 100 150 200 250 300
Location on female genetic map (cM)
Pro
geny
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MLEs of interference parameter
0
5
10
15
1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22 X
Chromosome
Inte
rfer
ence
par
amet
er
FemaleMale
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Goodness of fit?
3456789
10111617
0 50 100 150 200 250 300
Location on female genetic map (cM)
Pro
geny
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Maternal chromosome 1
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Paternal chromosome 1
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Maternal chromosome 2
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Paternal chromosome 2
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Mouse data
�
http://www.jax.org/resources/documents/cmdata/ftp.html
� Two interspecific backcrosses with common F1 parent
– BSB: (C57BL/6J � M. spretus) � C57BL/6J– BSS: (C57BL/6J � SPRET/Ei) � SPRET/Ei– 94 individuals from each cross
� High-density STRP markers
– BSB: 1372 markers– BSS: 4913 markers
� Average spacing:
– BSB: 1.0 cM– BSS: 0.3 cM
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Backcross pedigree
B S
F1 S
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Mouse data
0 20 40 60 80 100
Chromosome position (cM)
Bac
kcro
ss in
divi
dual
s
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MLEs: mouse
Chromosome
1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 X
Inte
rfer
ence
par
amet
er
1
2
4
8
16
32
64
128
256
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Crossover locations: Chr 1
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Crossover locations: Chr 4
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Inter-XO distances: Chr 1
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Inter-XO distances: Chr 4
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Acknowledgements
Terry Speed, University of California, Berkeley, and WEHI
Hongyu Zhao, Yale University
Mary Sara McPeek, University of Chicago
Jim Weber, Marshfield Medical Research Foundation
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References
� McPeek MS (1996) An introduction to recombination and linkage analysis. In:Speed TP, Waterman MS (eds) Genetic mapping and DNA sequencing. IMAvolumes in mathematics and its applications. Vol 81. Springer-Verlag, NewYork, pp 1–14
� McPeek MS, Speed TP (1995) Modeling interference in genetic recombination.Genetics 139:1031–1044
� Zhao H, Speed TP, McPeek MS (1995) Statistical analysis of crossover interfer-ence using the chi-square model. Genetics 139:1045–1056
� Zhao H, McPeek MS, Speed TP (1995) Statistical analysis of chromatid inter-ference. Genetics 139:1057–1065
� Speed TP (1996) What is a genetic map function? In: Speed TP, Waterman MS(eds) Genetic mapping and DNA sequencing. IMA volumes in mathematics andits applications. Vol 81. Springer-Verlag, New York, pp 65–88
� Zhao H, Speed TP (1996) On genetic map functions. Genetics 142:1367–1377
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� Broman KW, Weber JL (2000) Characterization of human crossover interfer-ence. Am J Hum Genet 66:1911–1926
� Broman KW, Rowe LB, Churchill GA, Paigen K (2002) Crossover interferencein the mouse. Genetics 160:1123–1131