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Summary Locating genes underlying human phenotypes

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  • February 21, 2022
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  • 2018/2019
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BLGY1232 Locating genes underlying human phenotypes

If the biochemical basis of the phenotype is known
 This usually means we know which enzyme is defective and we know something
about the polypeptide sequence of the enzyme
 The protein sequence can be used in a genome database search to identify the
gene sequence in the human genome allowing us to PCR-amplify the dene for
affect and unaffected individuals and identify any mutation in the affected
individuals and their families to see if they are also at risk
 Haemoglobin in haemoglobinopathies, Hexosaminidase A in Tay-Sachs disease,
Apolipoprotein E in typeIII hyperlipidaemia, Cystic fibrosis etc.

If we don’t know the biochemical basis of a condition
 We have to locate where the gene is in the genome, identify the correct coding
sequence and determine the nature of the mutation and its effect on the protein
encoded
 2 statistical approaches can be used; analysis based on genetic linkage or
analysis based on allelic association  both rely on genetic variation
(polymorphisms) between individuals
 To locate the gene, we need to know where it lies in the genome in relation to
other known sequences that differ between individuals - We need to analyse
how it relates to other polymorphisms and the key point is that the variant
sequence should be maintained within a proportion of the population: it’s not
just a one-off mutation
 Polymorphism = The existence of two or more variants (alleles, phenotypes, DNA
sequence variants, chromosome structural variations) at significant frequencies
in the population

Autozygosity mapping
 Pedigree analysis in families with a high incidence of consanguineous marriage
 Where parents are related, there is a higher frequency of autosomal recessive
inherited disorders
 They are obviously homozygous or the causal mutation, but they will also likely
be homozygous for a large region of the chromosome around this
 We can try and determine the genotypes of affected individuals and their family
members, to identify the genetic interval within which the disease gene lies; this
region will be homozygous in affected and heterozygous in unaffected family
members

Generally, any genetic variant allele that exists at or above a frequency of 1% of the
population is considered to be a polymorphism.

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