Download Early cleavage stages

Survey
yes no Was this document useful for you?
   Thank you for your participation!

* Your assessment is very important for improving the workof artificial intelligence, which forms the content of this project

page
1
page
2
page
3
page
4
page
5
page
6
page
7
page
8
page
9
page
10
page
11
page
12
page
13
page
14
page
15
page
16
page
17
page
18
page
19
page
20
page
21
page
22
page
23
page
24
Document related concepts

Epigenetics of human development wikipedia , lookup

Protein moonlighting wikipedia , lookup

Gene expression profiling wikipedia , lookup

Point mutation wikipedia , lookup

Nicotinic acid adenine dinucleotide phosphate wikipedia , lookup

Epigenetics of neurodegenerative diseases wikipedia , lookup

Polycomb Group Proteins and Cancer wikipedia , lookup

Non-coding RNA wikipedia , lookup

Polyadenylation wikipedia , lookup

Mir-92 microRNA precursor family wikipedia , lookup

Primary transcript wikipedia , lookup

RNA-binding protein wikipedia , lookup

NEDD9 wikipedia , lookup

Messenger RNA wikipedia , lookup

Epitranscriptome wikipedia , lookup

Transcript 
Drosophila and Syncitial
Specification
Early Cleavage Stages
• Syncytial blastoderm
– Superficial cleavage
– 13 cycles of rapid nuclear divisions (8 min)
– Each nucleus surrounded by microtubules and
microfilaments
– Future germ cells cellularize first (pole cells)
• Cellular blastoderm
– 6000 cells
– 4 hrs. post fertilization
Nuclear Migration
Segmentation of Embryo and Adult
What Specifies A-P Segmentation?
• How does this pattern arise?
• How are anterior-posterior and dorsal-ventral axes
established?
• How is a segmented pattern generated along the
anterior-posterior axis?
• How is each segment differentiated from the
others?
What is the Evidence for Early
Polarity
• Anterior half and posterior half of embryo have different
potentials shortly after fertilization
– ligation experiments
• Cut in half gives ends but no middles
– “organizing centers” at anterior and posterior ends?
– interference with anterior organizing center
• UV or RNase
• embryos lack head and thorax
• develop mirror symmetric abdomen and ends
• Suggests “morphogens” that exist in concentration
gradients
• What are the morphogens?
How Do You Find the
Morphogens Genetically?
• Christiane Nusslein-Volhard began a genetic approach
(1980s)
• Identify (screen for) mutations that cause defects in
embryonic polarity and classify
– Maternal-effect
• bicoid, hunchback (embryo with no head and thorax region)
• nanos, caudal (embryo with no posterior abdominal region)
• torso, torso-like (embryo with no ends)
– Zygotic-effect
• Regulated by above
A Maternal Anterior
Determinant: Bicoid
• bicoid mutant
phenotype:
• bicoid mRNA is
placed into the
oocyte
asymmetrically
• mRNA attaches
to microtubules
in anterior
Oogenesis Polarity
• Adult ovariole:
Mechanism of Bcd
mRNA
Localization
How Does Bicoid Get To
Anterior?
• Oocyte gerkin protein tells terminal follicle cells to be
posterior
• Posterior follicle cells signal to activate protein kinase A in
oocyte membrane
• Controls MT orientation (+ end toward posterior)
• Bicoid mRNA 3’ UTR binds to exuperantia and swallow
that bind to dynein
– go to anterior
• (Other mRNAs bind to kinesin)
– to go to posterior)
Where is Bicoid Protein Found?
Protein gradient is more extensive than mRNA
Translation occurs after fertilization
Comparison of Gradients
What Happens if mRNA Is Misplaced?
• Evidence that BCD is sufficient to initiate anterior
development:
What Happens If Gradient Shape
Is Altered?
• Evidence that BCD
concentration is important
for placement of segments
• swallow and exuperantia
mutants:
– BCD gradient is not as
sharp
• Or overexpress bcd
ant
post
wt
A H T Ab Te
exu
H
T
Ab Te
A Maternal Posterior
Determinant: Nanos
• nanos phenotype is opposite
of bicoid:
– Required for posterior
development
• mRNA is
asymmetrically
localized
– At posterior end
– Kinesin bound oskar
mRNA and staufen protein
– Staufen allows translation
of oskar which binds
nanos mRNA at posterior
– Nanos protein gradient
What Do Morphogens Do?
• bicoid and nanos regulate gene expression of other
maternal RNAs:
– hunchback
– caudal
What Do Morphogens Do?
• Bicoid inhibits
translation of caudal
mRNA
• Nanos inhibits
translation of
hunchback
Setting Up AP Gradients
What Do Morphogens Do?
• 2 ant -> post
gradients
• 2 post -> ant
gradients of
proteins
• bicoid, caudal,
hunchback act as
transcriptional
regulators of
zygotic genes
A Third Set of Maternal mRNAs:
Terminal Genes
• Terminal group: torso and torso-like
– mutants lack extreme anterior and posterior
structures (acron and telson)
What Type of Protein is Torso?
• Made in ovarian cells and mRNA placed
into oocyte
– torso RNA and protein are evenly distributed
– torso = RTK, a transmembrane protein
• Constitutive mutant (always on) converts
whole anterior to acron and posterior to
telson
– So must be spatially activated
What Activates Torso?
• Torso-like
• Not expressed in
oocyte, but in follicle
cells
• Only in anterior
and posterior
• Protein secreted and
activates torso locally
What Does Torso Signal?
• Torso RTK causes phosphorylations that
ultimately inactivate groucho protein
• Groucho is transcriptional inactivator of
some zygotic genes needed for specification
of ends
• Inhibiting an inhibitor activates
Related documents
PowerPoint of Drosophila Development 101
PowerPoint of Drosophila Development 101
Maternal Effect Genes
Maternal Effect Genes
File
File
Maternal effect genes
Maternal effect genes
Maternal effect genes
Maternal effect genes
Maternal effect genes
Maternal effect genes
Drosophila A
Drosophila A
Bicoid mRNA - bthsresearch
Bicoid mRNA - bthsresearch
messenger RNA (mRNA)
messenger RNA (mRNA)
Evidence for determination of the blastoderm
Evidence for determination of the blastoderm
Heart Dissection 101
Heart Dissection 101
Heart Dissection Pre-Lab
Heart Dissection Pre-Lab