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Genetic linkage analysis Dotan Schreiber According to a series of presentations by M. Fishelson.

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Presentation on theme: "Genetic linkage analysis Dotan Schreiber According to a series of presentations by M. Fishelson."— Presentation transcript:

1 Genetic linkage analysis Dotan Schreiber According to a series of presentations by M. Fishelson

2 OutLine Introduction. Basic concepts and some background. Motivation for linkage analysis. Linkage analysis: main approaches. Latest developments.

3 “Genetic linkage analysis is a statistical method that is used to associate functionality of genes to their location on chromosomes.“ http://bioinfo.cs.technion.ac.il/superlink/

4 The Main Idea/usage: Neighboring genes on the chromosome have a tendency to stick together when passed on to offsprings. Therefore, if some disease is often passed to offsprings along with specific marker- genes, then it can be concluded that the gene(s) which are responsible for the disease are located close on the chromosome to these markers.

5 Basic Concepts Locus Allele Genotype Phenotype

6 Dominant Vs. Recessive Allele דוגמא קלאסית: צבע עיניים homozygote heterozygote

7 (se)X-Linked Allele Most human cells contain 46 chromosomes: 2 sex chromosomes (X,Y): XY – in males. XX – in females. 22 pairs of chromosomes named autosomes. Around 1000 human alleles are found only on the X chromosome.

8 “…the Y chromosome essentially is reproduced via cloning from one generation to the next. This prevents mutant Y chromosome genes from being eliminated from male genetic lines. Subsequently, most of the human Y chromosome now contains genetic junk rather than genes.” http://anthro.palomar.edu/biobasis/bio_3b.htm

9 Medical Perspective When studying rare disorders, 4 general patterns of inheritance are observed: Autosomal recessive (e.g., cystic fibrosis). –Appears in both male and female children of unaffected parents. Autosomal dominant (e.g., Huntington disease). –Affected males and females appear in each generation of the pedigree. –Affected parent transmits the phenotype to both male and female children.

10 Continued.. X-linked recessive (e.g., hemophilia). –Many more males than females show the disorder. –All daughters of an affected male are “carriers”. –None of the sons of an affected male show the disorder or are carriers. X-linked dominant. –Affected males pass the disorder to all daughters but to none of their sons. –Affected heterozygous females married to unaffected males pass the condition to half their sons and daughters.

11 Example –After the disease is introduced into the family in generation #2, it appears in every generation  dominant! –Fathers do not transmit the phenotype to their sons  X-linked! 1 2345678910

12 Crossing Over Sometimes in meiosis, homologous chromosomes exchange parts in a process called crossing-over, or recombination.

13 Recombination Fraction The probability  for a recombination between two genes is a monotone, non- linear function of the physical distance between their loci on the chromosome.

14 Linkage The further apart two genes on the same chromosome are, the more it is likely that a recombination between them will occur. Two genes are called linked if the recombination fraction between them is small (<< 50% chance)

15 Linkage related Concepts Interference - A crossover in one region usually decreases the probability of a crossover in an adjacent region. CentiMorgan (cM) - 1 cM is the distance between genes for which the recombination frequency is 1%. Lod Score - a method to calculate linkage distances (to determine the distance between genes).

16 Ultimate Goal: Linkage Mapping With the following few minor problems: –It’s impossible to make controlled crosses in humans. –Human progenies are rather small. –The human genome is immense. The distances between genes are large on average.

17 Possible Solutions Make general assumptions: Hardy-Weinberg Equilibrium – assumes certain probability for a certain individual to have a certain genotype. Linkage Equilibrium – assumes two alleles at different loci are independent of each other. Incorporate those assumptions into possible solutions: Elston-Stewart method. Lander-Green method.

18 Elston-Stewart method Input: A simple pedigree + phenotype information about some of the people. These people are called typed. Simple pedigree – no cycles, single pair of founders. founder leaf 1/2

19 ..Continued Output: the probability of the observed data, given some probability model for the transmission of alleles. Composed of: founder probabilities - Hardy-Weinberg equilibrium penetrance probabilities - The probability of the phenotype, given the genotype transmission probabilities - the probability of a child having a certain genotype given the parents’ genotypes

20 ..Continued Bottom-Up: sum conditioned probabilities over all possible genotypes of the children and only then on the possible genotypes for the parents. Linear in the number of people.

21 Lander-Green method Computes the probability of marker genotypes, given an inheritance vector. P(Mi|Vi) at locus i marker data at this locus (evidence). A certain inheritance vector.

22 Main Idea Let a = (a 1,…,a 2f ) be a vector of alleles assigned to founders of the pedigree (f is the number of founders). We want a graph representation of the restrictions imposed by the observed marker genotypes on the vector a that can be assigned to the founder genes. The algorithm extracts only vectors a compatible with the marker data. Pr[m|v] is obtained via a sum over all compatible vectors a.

23 Example – marker data on a pedigree 12 1211 a/b 21 13 22 14 a/b 2324 b/d a/c

24 Example – Descent Graph 12 1211 a/b 21 13 22 14 a/b 2324 b/d a/c 3456 1278 (a,b) (a,c)(b,d)(a,b) Descent Graph

25 3456 1278 (a,b) (a,c)(b,d)(a,b) Descent Graph 1. Assume that paternally inherited genes are on the left. 2. Assume that non-founders are placed in increasing order. 3.A ‘1’ (‘0’) is used to denote a paternally (maternally) originated gene.  The gene flow above corresponds to the inheritance vector: v = ( 1,1; 0,0; 1,1; 1,1; 1,1; 0,0 )

26 Example – Founder Graph 53 21 64 87 (b,d) (a,b) (a,c) (a,b) Founder Graph 3456 1278 (a,b) (a,c)(b,d)(a,b) Descent Graph

27 Find compatible allelic assignments for non-singleton components 1.Identify the set of compatible alleles for each vertex. This is the intersection of the genotypes. 53 21 64 87 (b,d) (a,b) (a,c) (a,b) {a,b} ∩ {a,b} = {a,b}{a,b} ∩ {b,d} = {b}

28 Possible Allelic Assignments 53 21 64 87 (b,d) (a,b) (a,c) (a,b) {a,b} {a,c} {a} {b} {b,d} {a,b,c,d} Allelic AssignmentsGraph Component (a), (b), (c), (d)(2) (a,b,a), (b,a,b)(1,3,5) (a,b,c,d)(4,6,7,8)

29 Computing P(m|v) If for some component there are no possible allelic assignments, then P(m|v) = 0. The probability of singleton components is 1  we can ignore them. Let a hi be an element of a vector of alleles assigned to the vertices of component Ci. over 2f elements 2 terms at most Linear in the number of founders

30 Latest News: SuperLink Combines the covered approaches in one unified program. Has other built-in abilities that increase its computations efficiency. Claimed to be more capable and faster than other related programs (by its own makers). http://bioinfo.cs.technion.ac.il/superlink/

31 The End


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