Functional analysis of DAZL-mediated translation activation during mammalian gametogenesis
dc.contributor.advisor
Gray, Nicola
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dc.contributor.advisor
Mcneilly, Alan
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dc.contributor.author
Sousa Martins, Joao Pedro
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dc.contributor.author
Martins, Joao Pedro
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dc.contributor.sponsor
Medical Research Council (MRC)
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dc.date.accessioned
2015-01-30T14:36:39Z
dc.date.available
2015-01-30T14:36:39Z
dc.date.issued
2012-11-30
dc.description.abstract
Gametogenesis is a highly complex process that requires stringent control of
gene expression, in which translational regulation plays an essential role. Deleted in
Azoospermia-like (DAZL) belongs to the DAZ family of RNA-binding proteins,
which are restricted to germ cells, and regulate mRNA translation. Importantly, loss
of function of these proteins results in infertility in both males and females in a wide
variety of organisms.
A model for the mechanism by which DAZL stimulates translation has been
proposed based on work in Xenopus laevis (X. laevis) oocytes. In this model, DAZL
functions by recruiting the translation initiation factor poly(A)-binding protein
(PABP) to the 3’ untranslated region (UTR) of messenger RNAs. Simultaneous
binding of PABP to Dazl and factors at the 5’ end confers a “closed-loop” mRNA
conformation, which promotes translation initiation.
To examine whether DAZL plays a similar role in mammals, co-expression
of Dazl and PABP family members was investigated in fetal and adult mouse
gonads. In contrast to X. laevis, mammals encode four cytoplasmic PABPs which
share a similar domain organisation: PABP1, tPABP, ePABP and PABP4, of which
PABP1 and PABP4 appear to be expressed in a wide range of tissues.
Immunohistochemistry revealed that Dazl, Pabp1 and Pabp4 are all expressed in
primordial germ cells (PGCs) but these show different expression patterns following
germ cell sex differentiation. In adult testes Dazl is expressed in spermatogonia and
spermatocytes, coinciding with the peak of Pabp4 expression. In contrast, the peak of
Pabp1 expression occurs later than that of Dazl, with these proteins only being co-expressed
in late pachytene and secondary spermatocyte phases. In adult ovaries,
Pabp1, Pabp4 and Dazl are all expressed in the oocytes of primordial and primary
follicles. Since both PABP family members are co-expressed with Dazl, the ability of
DAZL to interact with PABP1 and PABP4 was investigated in vitro and in vivo.
Surprisingly, these studies showed that DAZL discriminates between different PABP
family members, only interacting with PABP1, providing the first report of a PABP-specific
protein partner. Several putative DAZL mutations have been identified in patients with
impaired fertility. Two of these mutations, I37A and R115G, are located in the RNA
recognition motif (RRM), a domain which is found in many RNA-binding proteins
and mediates both RNA and protein interactions. Thus, the role of these mutations in
the ability of DAZL to stimulate translation was investigated. To this end, a
translational target of human DAZL (hDAZL) was sought. The 3’UTR of growth
differentiation factor 9 (hGDF9) mRNA was found to confer regulation by hDAZL
and thus the ability of mutant DAZLs to stimulate reporter mRNAs containing this
3’UTR was examined. This revealed that both mutations compromised the ability of
hDAZL to stimulate hGDF9 translation, suggesting a causative effect. These results
were further confirmed in assays in which hDAZL is artificially tethered to mRNAs.
The ability of mutant hDAZLs to stimulate translation in this assay was
compromised suggesting that loss of function is, at least in part, due to impaired
protein-protein interactions rather than altered RNA-binding.
This work provides insights into the molecular mechanism by which DAZL
stimulates the translation of specific mRNAs during mammalian gametogenesis and
provides evidence that this function may play an important physiological role in
human reproduction.
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dc.identifier.uri
http://hdl.handle.net/1842/9893
dc.language.iso
en
dc.publisher
The University of Edinburgh
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dc.relation.hasversion
Gorgoni B, Richardson WA, Burgess HM, Anderson RC, Wilkie GS, Gautier P, Sousa Martins, JP, Brook M, Sheets MD, Gray NK. (2011) Poly(A)-binding proteins are functionally distinct and have essential roles during vertebrate development. Proc Natl Acad Sci U S A. 10;108(19):7844-9.
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dc.subject
DAZL
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dc.subject
Deleted in Azoospermia-like
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dc.subject
gametogenesis
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dc.subject
PABP
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dc.title
Functional analysis of DAZL-mediated translation activation during mammalian gametogenesis
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dc.type
Thesis or Dissertation
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dc.type.qualificationlevel
Doctoral
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dc.type.qualificationname
PhD Doctor of Philosophy
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