Mapping Mendelian Disease Flashcards

1
Q

What is the definition of Mendelian disease?

A

→ A disease caused by a single gene with little or no impact from the environment

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2
Q

What is an example of mendelian disease?

A

→ PKD

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3
Q

What is the definition of non mendelian disease?

A

→ Diseases or traits caused by the impact of many different genes each having only a small individual impact on the final condition

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4
Q

What is an example of a non mendelian disease?

A

→ Psoriasis

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5
Q

What is the definition of a multifactorial disease?

A

→ Diseases or traits resulting from an interaction between multiple genes and often multiple environmental factors

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6
Q

What is an example of a multifactorial disease?

A

→ heart disease

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7
Q

What are the 3 ways of identifying a gene by mapping?

A

→ Homozygosity mapping
→ Linkage analysis

→ GWAS

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8
Q

How do you find disease causing mutations?

A

→ Sequencing

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9
Q

How do you prove genes cause disease?

A

In silico, in vitro and in vivo tools

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10
Q

What is genetic linkage?

A

→ The tendency for alleles at neighbouring loci to be segregated together at meiosis

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11
Q

When are crossovers more likely to occur?

A

→ between loci separated by some distance than those close together

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12
Q

If a marker and a disease locus are unlinked what does this mean?

A

→ The affected individuals in the family are less likely to inherit the same marker alleles

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13
Q

If a marker and a disease locus are linked what does this mean?

A

→ Affected individuals are more likely to inherit this haplotype block

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14
Q

What are the steps for the linkage analysis method?

A

1) a pedigree is taken
2) genotyping data is generated like a GWAS SNP array

3) Physical and genetic distribution of markers on genotypic array
4) a file is generated with pedigree information and genotyping data from microarray
5) linkage programme is run

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15
Q

What is non parametric linkage testing?

A

→ Not having assumptions about linkage data

→No rules imposed in NPL –inheritance pattern is not taken into consideration

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16
Q

What does non parametric linkage testing look for?

A

→ All affected regions are equal but different to unaffected regardless of inheritance pattern
→ Any LOD score above 3

17
Q

What does parametric analysis look for?

A

→ All affected are equal but different to unaffected

→ AND genotypes follow the imposed inheritance pattern

18
Q

What does a LOD score of -2 mean?

A

→ significant non linkage

19
Q

What does a LOD score of -2 to 3 mean?

A

→ Inconclusive

20
Q

Where is a gene likely to be located if the LOD score is ?> 3?

A

→ between the two markers defining the linkage peak

21
Q

What are the symptoms of generalised lymphatic dysplasia?

A

→ Antenatal hydrops
→ Oedematous at birth

→ intestinal lymphangiectasia
→ peripheral lymphoedema
→ mild developmental delay

22
Q

What kind of a disease is 4 limb lymphoedema?

A

→ autosomal dominant

23
Q

What are the two methods of finding disease causing mutations?

A

→ Traditional Sanger sequencing
→ Next generation sequencing

  • whole genome
  • whole exome
24
Q

What are the black areas on SNP arrays?

A

represent gaps in the human genome sequence, primarily centromeres and teleomeres

25
Q

How is parametric analysis different from NPL?

A

imposes rules about inheritance and disease frequency

26
Q

What rules would you apply to autosomal dominant for parametric analysis?

A

→apply a rule for affected family members to be heterozygous

27
Q

What rules would you apply to autosomal recessive for parametric analysis?

A

→apply a rule for affected family members to be homozygous for the mutant allele

28
Q

What are the features of 4-limb lymphedema?

A

→Pubertal/adult onset
→Associated with venous incompetence
→No other abnormalitie

29
Q

If two alleles are on the same chromosome, are they always linked and inherited together?

A

→Alleles are not always inherited together. This depends on how far apart the genes
→There is an equal likelihood of them being inherited together or separated during crossing over – there is linkage equilibrium.