L4- multifactorial disease Flashcards

1
Q

What is meant by the term Mendelian?

A

Means that a certain disease obeys Mendel’s laws of segregation for example it being: dominant, recessive, X-linked

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2
Q

What is meant by the term Complex?

A

Describes something with an inherited but non-Mendelian component

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3
Q

What is meant by the term Polygenic?

A

The result of the action of multiple genes

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4
Q

What is meant by Multifactorial?

A

the result of multiple factors, usually including both genetic and environmental factors

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5
Q

Useless question?: What does the sign Lambda s mean?

A

Relative risk to 2nd sibling

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6
Q

Does a multifactorial disease have a genetic

component? Example of twin studies…

A

Twin studies: genetic characters should have a higher concordance in monozygotic (MZ) twins compared to dizygotic (DZ) twins

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7
Q

What are the issues with twin studies?

A
  • large differences in birth weight for MZ twins (ie differences in prenatal environment of each twin)
  • variation in the time of splitting of the early embryo
  • diamniotic monozygotics (with separate amniotic cavities) survive much better than monochorionic
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8
Q

Issues with adoptive studies?

A

-child is put into a totally different environment to its birth environment because of adoption

  • share genes but not environments with the biological parents
  • share environments but not genes with their adoptive parents
  • BUT still share uterine environment
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9
Q

What are the human characteristics with multifactorial Inheritance?

A
  • Phenotypes determined by action of many genes at different loci
  • Genes are not dominant or recessive but additive
  • Includes many human traits/common diseases; blood pressure, head circumference, height, intelligence
  • traits tend to be normally-distributed in the general population ie forms a Gaussian “bell-shaped curve”
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10
Q

Examples of disorders which show multifactorial inheritance

A

-Congenital malformations: cleft lip/palate, congenital hip dislocation, congenital heart defects, neural tube defects, pyloric stenosis, talipes

-Acquired diseases of childhood & adult life:
asthma, autism, cancer, diabetes mellitus, epilepsy, glaucoma, hypertension, inflammatory bowel disease (Crohn disease), ischaemic heart disease & stroke, bipolar disorder, multiple sclerosis, Parkinson disease, psoriasis, rheumatoid arthritis, schizophrenia

-Effect of the environment
E.g like NTD (neural tube defects) maternal folic acid insufficiency

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11
Q

What is the purpose of Genetic association studies ?

A

To relate variation in human DNA sequence with a disease or trait

Association method provides greater power to detect common genetic variants conferring susceptibility to complex phenotypes
Estimates population attributable risk

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12
Q

Frequency in population vs magnitude of effect of multifactorial traits/diseases

A

see slide 15

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13
Q

Linkage disequilibrium can occur in population association studies …why?

A

Because most disease bearing chromosomes in population are descended from one (or a few) ancestral chromosomes, therefore present day individuals can be affected by these chromosomes

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14
Q

Alzheimer’s Disease

A

most common form of dementia >40 yr

symptoms: inability to cope, loss of memory, brain damage
neurology: shrinkage of brain, tangles of b-amyloid protein in nerve fibres of hippocampus

Important genes: presenilin 1 (PSEN1) and presenilin 2 (PSEN2) for transmembrane aspartyl-proteases

g-secretase activity responsible for proteolytic cleavage of amyloid beta A4 precursor protein (APP) and NOTCH receptor proteins

missense mutations in APP lead to a build up

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15
Q

APOE haplotypes

A

APOE has three haplotypes: APOEE2, APOEE3, and APOE*E4

*E4 haplotype confers increase in susceptibility
*E2 haplotype confers a protective effect
E4/E4 homozygotes are affected much earlier than heterozygotes

E2/E3 vs. E4/E4:
risk for late-onset AD increases 20 → 90%
mean age of onset decreases 84 → 68 years
risk is increased still further if there is high blood pressure

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16
Q

Age-related Macular Degeneration

A

Leading cause of irreversible central visual dysfunction caused by degeneration of the macula
Characterized by the early deposition of drusen, a hallmark risk factor for AMD

Genetics
1) Major effects; CFH (1q), ARMS2 (10q)

2) Environment
Major effect; smoking
Intermediate effect; light exposure.

= approximately 70 fold increase in risk