Personalized Medicine Flashcards

1
Q

clinical application of NGS

A

rare undiagnosed diseases

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2
Q

pathogen variants __ with phenotype, ___ do not.

A

pathogenic variants segregate with phenotype, benign variants do not.

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3
Q

Is variant polymorphic in “normal” population?

A

requires accurate DBs with large control populations

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4
Q

Is variant de novo in the proband, or inherited from a phenotypically normal parent?

A

presumes variant is fully penetrant.

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5
Q

how do we focus on the variants that are clinically significant?

A

penetrance assumption
inheritance hypotheses
candidate genes/context
effect/functional/evolutionary predictions.

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6
Q

databases: caveat emptor

A

databases are incomplete
the upstream literature is incomplete.
numerous errors in databases.

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7
Q

true or false: loss of function indicates a disease

A

false

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8
Q

false-positive and false-negative variant calles increase with the

A

size of the sequenced target (gene > exome > genome)

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9
Q

Takahashi’s experiment

A

he took skin cells from adult mice and infected them with a virus to introduce 24 genes. The cells transformed, and looked and behaved like pluripotent embryonic stem cells.

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10
Q

What the cells (ES like cells, or pluripotent stem cells) from Takahashi’s experiment were called

A

induced pluripotent stem cells, or iPS cells.

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11
Q

iPS cells are important for

A

modelling and investigating human diseases, as well as for screening drugs.

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12
Q

A prolbem with iPS cells is

A

consistency - some people have done something remarkable with one cell line, and it turns out nobody else can do it.

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13
Q

genes responsible for reprogramming adult cells into iPS cells

A

oct3/4
sox2
Klf4
c-myc.

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14
Q

scientists discovered that iPS cells retain an

A

epigenetic memory: a pattern of chemical marks on their DNA that reflects their original cell type. Such changes should not affect the cells’ use in therapies.

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15
Q

The reslt of implanting retinal pigment epithelium from iPS cells in a patient with macular degeneration was

A

a halt in the patient’s macular degeneration.

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16
Q

most iPS reprogramming teachiques are

A

inefficient: only a small fraction of cells end up fully reprogrammed. iPS cells vary from one strain to another. That has made it hard to establish controls in experiments.

17
Q

CRISPR-Cas9 gene editing tool, has enabled researchers to

A

introduce disease associated mutations into a sample of iPS cells and then comparethem with the original, unedited cell lines.

18
Q

because iPS cells resemble embryonic cells, they are not always ideal for

A

studying late-onset diseases such as dementia.

19
Q

iPS cells have also been used with some success in

A

drug discovery: they provide a plentiful source of patient derived cells to screen or test experimental drugs.