Role of TrkB in neonatal ovary development
dc.contributor.advisor
Spears, Norah
en
dc.contributor.advisor
Price, David
en
dc.contributor.author
Lannagan, Tamsin R. M.
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dc.date.accessioned
2010-11-03T09:42:23Z
dc.date.available
2010-11-03T09:42:23Z
dc.date.issued
2009
dc.description.abstract
The signalling cascade induced by the binding of neurotrophins (NGF,
BDNF, NT3 and NT4) to their high-affinity tyrosine kinase receptors
(TrkA, B and C) is well documented to be important for neuronal cell
survival, proliferation and differentiation. Evidence has accumulated
demonstrating the importance of these signalling pathways in nonneuronal
tissues, including the ovary where all neurotrophins and their
receptors are expressed. In the mouse, effects on ovulation have been
demonstrated but the role of Trk signalling in neonatal ovary
development is less clear. Previous work had found that TrkB
expression is upregulated at the time of follicle formation in the mouse
and transgenic mice null for the TrkB receptor demonstrate significant
loss of oocytes neonatally (TrkB knockouts, KO, die shortly after birth).
This thesis examines the phenotype of the TrkB KO using
morphological, histological and surgical techniques with the aim being
to further investigate the role of TrkB signalling in oocyte survival, and
to contribute to our understanding of neonatal ovary development. The
main questions addressed are: 1) what developmental defects are
occurring on a morphological level that result in the phenotype of the
TrkB KO; 2) can these defects be quantified; and 3) what are the longterm
survival prospects for TrkB KO oocytes. Morphological assessment
revealed that TrkB KO ovaries exhibit poorer follicle health than their
Controls and this was confirmed by assessment of basement membrane
(BM) composition. TrkB KO brain and kidney were also assessed and
found to have similarly affected BM. It is well known that cells require
contact with the BM to maintain survival, thus it is postulated that TrkB
signalling contributes to oocyte survival through regulation of the BM.
Due to the postnatal lethality of the mutation, TrkB KO ovaries were
transplanted to ascertain long-term oocyte survival. Unexpectedly it
was found that TrkB KO oocytes are able to survive and follicles grow as well as they do in the Control transplants. Consequently, the in vivo
effect has to be indirect. It is known that oocytes in the neonatal ovary
undergo an increased rate of cell death but it is not known how the cell
debris is removed. A novel observation of a neonatal ovarian immune
response has been made in this thesis and is postulated to be a
physiological mechanism for cell debris clearance. In conclusion, this
thesis has demonstrated that signalling through TrkB has an effect on
regulating BM in the ovary and other organs, but that surprisingly it has
an indirect effect on oocyte survival.
en
dc.identifier.uri
http://hdl.handle.net/1842/4147
dc.language.iso
en
dc.publisher
The University of Edinburgh
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dc.subject
mouse ovary
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dc.subject
oocyte
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dc.subject
TrkB
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dc.subject
KO
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dc.subject
basement membrane
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dc.subject
ovarian transplantation
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dc.subject
immune response
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dc.title
Role of TrkB in neonatal ovary development
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dc.type
Thesis or Dissertation
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dc.type.qualificationlevel
Doctoral
en
dc.type.qualificationname
PhD Doctor of Philosophy
en
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