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Transcript
Mosaic screens
Reading: pages 702-707
lecture notes
white can be used as cell autonomous
marker to monitor the loss of sev.
Analyze ommatidia at the periphery of mutant clone.
These will be mosaic, containing both wild-type and mutant cells.
Mutant clone
Approaches to identifying genes
involved in development.
1. Direct screens: will often fail to identify essential
genes required earlier in development (exceptionhypomorphic mutations).
2. Sensitized screens: enhancer screens.
3. FLP/FRT mosaic screens.
Yeast 2 micron plasmid encodes a FLP
recombinase and two FRT sites.
FLP
FRT
FRT
X
FLP recombinase stimulates recombination
between two FRT sites.
FRT
FRT
Since replication origin fires only once during cell cycle.
Intramolecular recombination is thought to increase
copy number of 2 micron plasmid.
FRT
Expression of FLP
recombinase can stimulate
mitotic recombination at
FRT sites.
P[w+]
FRT
P[w+]
replication
P[w+]
P[w+]
X
Mitotic
crossing over
P[w+]
FLP recombinase expressed from the eyeless promoter
results in recombination just in the developing eye.
A digression
Mutations in two types of genes can lead to cancer
1. Oncogenes
Positive regulators of the cell proliferation
Activating mutations
2. Tumor suppressor genes
Negative regulators of cell proliferation
Loss-of-function mutations
Tumor suppressor genes can either inhibit
cell proliferation or promote cell death.
Tumor suppressor genes
Tumor suppressor genes
Cell proliferation
Cell death
Retinoblastoma is cancer of cone cells that is inherited as an
autosomal dominant trait.
Sporadic Rb-cancer in one eye
Inherited Rb-cancer in both eyes
3% inherited cases have deletion
in 13q14
In 1971 Knudson proposed that
in inherited forms of Rb a second
mutation occurred spontaneously
in the normal gene. In other
words, while Rb is inherited as a
dominant trait, it is recessive at
the cellular level.
How would I identify a
tumor
suppressor gene in
QuickTime™ and a
decompressor
are needed to seeDrosophila?
this picture.
QuickTime™ and a
decompressor
are needed to see this picture.
How to identify a tumor suppressor gene in
Drosophila?
eyFLP w y
w
eyFLP w y
w
FRT
m
FRT
m
FRT
m
X
FRT
If m is in tumor suppressor gene, white
cell will produce more cells than red cell
P[w+]
eyFLP w y
w
FRT
P[w+]
FRT
P[w+]
To screen for tumor suppressor genes, mutagenize and
look for mutants with excessive white tissue.
EMS
w
FRT
males
FRT
X
w
w
Balancer
females
Mutagenized chromosome
w
F1
or
w
FRT
Balancer
Cross individual F1 females
w
F1
w
FRT
m
Balancer
Some chromosomes will
have mutations in tumor
suppressor genes.
female
X
eyFLP w
FRT
P[w+]
FRT
P[w+]
males
F2 progeny
w/o balancer
eyFLP w
FRT
m
w
FRT
P[w+]
F2 progeny
w/o balancer
eyFLP w
FRT
w
FRT
m
X
P[w+]
eyFLP w
FRT
m
eyFLP w
FRT
P[w+]
w
FRT
m
w
FRT
P[w+]
If m is in tumor suppressor gene, white
cell will produce more cells than red cell
Screen for mutations on each chromosome
(FRT near centromere for each chromosome arm)
Mutations define 23 genes
Some were known tumor suppressor genes
that had been identified in humans.
Others were new genes, and their human homolgs
were found to be mutated in cancer cells.
QuickTime™ and a
decompressor
are needed to see this picture.