28 citations found with entrez 4/28/97
Genes Dev 11 (4): 423-435 (1997)
An Egalitarian-BicaudalD complex is essential for oocyte specification
and axis determination in Drosophila.
Mach JM, Lehmann R
Whitehead Institute for Biomedical Research and Department of Biology,
Massachusetts Institute of Technology, Cambridge 02142, USA.
Genetic experiments suggest that polarization of the oocyte is linked directly
to the initial cell fate determination that singles out the oocyte from
its 15 sister cells. Specification of oocyte cell fate as well as establishment
and maintenance of a polarized microtubule network within the Drosophila
oocyte require the activity of the egalitarian (egl) and BicaudalD (BicD)
genes. We have isolated the egl gene and show that Egl protein colocalizes
with BicD protein at all stages of oogenesis. Immunoprecipitation experiments
show that both proteins are part of a protein complex. Egl and BicD proteins
localize to the oocyte in three stages that correlate with the stepwise
polarization of the oocyte. We propose that the Egl-BicD protein complex
links microtubule polarity and RNA transport. During early oogenesis, the
complex is required to transport factors promoting oocyte differentiation;
during later stages of oogenesis the complex directs the sorting of RNA
molecules required for anterior-posterior and dorsoventral patterning of
the embryo.
Development 122 (12): 3863-3879 (1996)
The neurogenic genes egghead and brainiac define a novel signaling
pathway essential for epithelial morphogenesis during Drosophila oogenesis.
Goode S, Melnick M, Chou TB, Perrimon N
Department of Genetics, Harvard Medical School, Boston, Massachusetts 02115,
USA. goode@rascal.med.harvard.edu
Notch (N) and other neurogenic genes have been implicated in two fundamental
processes, lateral specification of cell fates, and epithelial development.
Previous studies have suggested that the neurogenic gene brainiac (brn)
is specifically required for epithelial development (Goode, S., Morgan,
M., Liang, Y-P. and Mahowald, A. P. (1996). Dev. Biol. 178, 35-50). In
this report we show that egghead (egh), a gene with phenotypes identical
to brn, encodes for a novel, putative secreted or transmembrane protein.
We describe the role of egh and brn germline function in the morphogenesis
of the follicular epithelium from the time it is born through the time
that it migrates towards the oocyte late in oogenesis. By comparing the
function of germline egh and brn to N during oogenesis, we have obtained
direct evidence for the involvement of Notch in maintenance of the follicle
cell epithelium, and the specificity of brn and egh in epithelial development
during oogenesis. The most striking phenotype observed for all three genes
is a loss of apical-basal polarity and accumulation of follicular epithelial
cells in multiple layers around the oocyte. The spatiotemporal onset of
this adenoma-like phenotype correlates with the differential accumulation
of egh transcripts in the oocyte at stage 4 of oogenesis. In contrast to
N, we find that brn and egh are essential for the organization, but not
specification, of stalk and polar cells. The expression patterns and functional
requirements of brn, egh, and N lead us to propose that these genes mediate
follicular morphogenesis by regulating germline-follicle cell adhesion.
This proposal offers explanations for (1) the involvement of egh and brn
in N-mediated epithelial development, but not lateral specification, (2)
why brn and egh embryonic neurogenic phenotypes are not as severe as N
phenotypes, and (3) how egh and brn influence Egfr-mediated processes.
The correlation between the differential expression of egh in the oocyte
and the differential requirement for brn, egh, and N in maintaining the
follicular epithelium around the oocyte, suggests that Egghead is a critical
component of a differential oocyte-follicle cell adhesive system.
Dev Biol 178 (1): 35-50 (1996)
Brainiac encodes a novel, putative secreted protein that cooperates
with Grk TGF alpha in the genesis of the follicular epithelium.
Goode S, Morgan M, Liang YP, Mahowald AP
Department of Molecular Genetics and Cell Biology, University of Chicago,
Illinois 60637, USA.
brainiac (brn) is involved in a number of developmental events. In addition
to being required zygotically for segregation of neuroblasts from epidermoblasts,
it is essential for a series of critical steps during oogenesis which also
depend upon gurken (grk), a TGF alpha homolog. Animals harboring strong
mutations of either grk or EGF receptor tyrosine kinase (Egfr) or doubly
mutant for brn and weak grk or Egfr mutations produce ovarian follicles
with multiple sets of nurse cell-oocyte complexes. These follicles frequently
have discontinuities in the follicular epithelium that uncover nurse cells
but not the oocyte. Gaps first appear in the germarium, suggesting that
some nurse cells lack affinity for invading prefollicular cells. This is
the first evidence that grk, in addition to its involvement in the genesis
of anterior-posterior and dorsal-ventral polarity, is also required for
Egfr-dependent development of the follicular epithelium that surrounds
each nurse cell/oocyte cluster to form an egg chamber. We have used restriction
fragment length polymorphisms to localize brn to a 10-kb region within
a 300-kb stretch of DNA on the X-chromosome, and we have identified the
brn gene by means of RNA rescue. brn codes for a putative secreted protein.
brn is expressed in germ cells at the time follicle cells first surround
the nurse cell-oocyte complex. Our genetic data suggest that brn acts in
a parallel, but partially overlapping pathway to the Grk-Egfr signaling
pathway. The brn pathway may help to provide specificity to TGF alpha -Egfr
function during oogenesis.
Development 121 (11): 3809-3818 (1995)
A small predicted stem-loop structure mediates oocyte localization
of Drosophila K10 mRNA.
Serano TL, Cohen RS
Department of Biochemistry, University of Kansas, Lawrence 66045, USA.
The establishment of dorsoventral polarity in the Drosophila oocyte and
future embryo is dependent on the efficient transport of K10 mRNA from
nurse cells into the oocyte. To investigate the cis-requirements of K10
mRNA transport, we used a transgenic fly assay to analyze the expression
patterns of a series of K10 deletion variants. Such studies identify a
44 nucleotide sequence within the K10 3' untranslated region that is required
and sufficient for K10 mRNA transport and subsequent localization to the
oocyte's anterior cortex. An inspection of the 44 nucleotide transport/localization
sequence (TLS) reveals a strong potential for the formation of a stem-loop
secondary structure. Nucleotide substitutions that interfere with the predicted
base-pairing of the TLS block mRNA transport and anterior localization.
Conversely, mutations that alter the base composition of the TLS while
maintaining predicted base-pairing do not block mRNA transport or anterior
localization. We conclude that K10 mRNA transport and anterior localization
is mediated by a 44 nucleotide stem-loop structure. A similar putative
stem-loop structure is found in the 3' untranslated region of the Drosophila
orb mRNA, suggesting that the same factors mediate the transport and anterior
localization of both K10 and orb mRNAs. Apart from orb, the K10 TLS is
not found in any other localized mRNA, raising the possibility that the
transport and localization of other mRNAs, e.g., bicoid, oskar and gurken,
are mediated by novel sets of cis- and trans-acting factors. Moreover,
we find that the K10 TLS overrides the activity of oskar cis-regulatory
elements that mediate the late stage movement of the mRNA to the posterior
pole. We propose the existence of a family of cis-regulatory elements that
mediate mRNA transport into the oocyte, only some of which are compatible
with the elements that mediate late stage movements.
Curr Biol 5 (11): 1252-1254 (1995)
Pattern formation. Gurken meets torpedo for the first time.
Gavis ER
Department of Molecular Biology, Princeton University, New Jersey 08544,
USA.
Intercellular communication between oocyte and follicle cells, mediated
by the gurken-torpedo/DER signalling pathway, has a crucial role in determining
both anterior-posterior and dorsal-ventral polarity in Drosophila.
Genes Dev 9 (20): 2482-2494 (1995)
Cappuccino, a Drosophila maternal effect gene required for polarity
of the egg and embryo, is related to the vertebrate limb deformity locus.
Emmons S, Phan H, Calley J, Chen W, James B, Manseau L
Department of Molecular and Cellular Biology, University of Arizona, Tucson
85721, USA.
We report the molecular isolation of cappuccino (capu), a gene required
for localization of molecular determinants within the developing Drosophila
oocyte. The carboxy-terminal half of the capu protein is closely related
to that of the vertebrate limb deformity locus, which is known to function
in polarity determination in the developing vertebrate limb. In addition,
capu shares both a proline-rich region and a 70-amino-acid domain with
a number of other genes, two of which also function in pattern formation,
the Saccharomyes cerevisiae BNI1 gene and the Aspergillus FigA gene. We
also show that capu mutant oocytes have abnormal microtubule distributions
and premature microtubule-based cytoplasmic streaming within the oocyte,
but that neither the speed nor the timing of the cytoplasmic streaming
correlates with the strength of the mutant allele. This suggests that the
premature cytoplasmic streaming in capu mutant oocytes does not suffice
to explain the patterning defects. By inducing cytoplasmic streaming in
wild-type oocytes during mid-oogenesis, we show that premature cytoplasmic
streaming can displace staufen protein from the posterior pole, but not
gurken mRNA from around the oocyte nucleus.
Oncogene 11 (6): 1033-1040 (1995)
Requirement of the ETS domain transcription factor D-ELG for egg chamber
patterning and development during Drosophila oogenesis.
Gajewski KM, Schulz RA
Department of Biochemistry and Molecular Biology, University of Texas MD
Anderson Cancer Center, Houston 77030, USA.
The D-elg gene encodes an ETS domain transcription factor that functions
in Drosophila oogenesis. D-elg belongs to a small group of genes that are
required for the formation of both the anteroposterior and dorsoventral
axes of the egg chamber. During oogenesis in D-elg mutant females, the
spatial localization of oskar and gurken mRNAs in the oocyte is disrupted
and a follicle cell enhancer trap marker identifies dorsoventral polarity
defects. Also, specialized follicle cells, called border cells, fail to
migrate from their anterior location to a position adjacent to the developing
oocyte. Consistent with these phenotypes, D-elg shows genetic interactions
with two genes required for normal egg chamber differentiation.
Cell 82 (5): 785-794 (1995)
An unusual mosaic protein with a protease domain, encoded by the nudel
gene, is involved in defining embryonic dorsoventral polarity in Drosophila.
Hong CC, Hashimoto C
Department of Genetics, Yale University School of Medicine, New Haven,
Connecticut 06520, USA.
Dorsoventral polarity of the Drosophila embryo is induced by a ventral
extracellular signal, which is produced by a locally activated protease
cascade within the extraembryonic perivitelline compartment. Local activation
of the protease cascade depends on a positional cue that is laid down during
oogenesis outside the oocyte. Here we present evidence that the nudel gene
encodes an essential component of this cue. The nudel gene, which is expressed
in follicle cells covering the oocyte, encodes an unusual mosaic protein
resembling an extracellular matrix protein with a central serine protease
domain. Our findings suggest that embryonic dorsoventral polarity is defined
by a positional cue that requires the nudel protein to anchor and to trigger
the protease cascade producing the polarity-inducing signal.
Development 121 (9): 3023-3033 (1995)
Mutations in the Drosophila gene bullwinkle cause the formation of
abnormal eggshell structures and bicaudal embryos.
Rittenhouse KR, Berg CA
University of Washington, Department of Genetics, Seattle 98195-7360, USA.
Subcellular localization of gene products and cell migration are both critical
for pattern formation during development. The bullwinkle gene is required
in Drosophila for disparate aspects of these processes. In females mutant
at the bullwinkle locus, the follicle cells that synthesize the dorsal
eggshell filaments do not migrate properly, creating short, broad structures.
Mosaic analyses demonstrate that wild-type BULLWINKLE function is required
in the germ line for these migrations. Since the mRNA for gurken, the putative
ligand that signals dorsal follicle cell fate, is correctly localized in
bullwinkle mutants, we conclude that our bullwinkle alleles do not affect
the dorsoventral polarity of the oocyte and thus must be affecting the
follicle cell migrations in some other way. In addition, the embryos that
develop from bullwinkle mothers are bicaudal. A KINESIN:beta-GALACTOSIDASE
fusion protein is correctly localized to the posterior pole of bullwinkle
oocytes during stage 9. Thus, the microtubule structure of the oocyte and
general transport along it do not appear to be disrupted prior to cytoplasmic
streaming. Unlike other bicaudal mutants, oskar mRNA is localized correctly
to the posterior pole of the oocyte at stage 10. By early embryogenesis,
however, some oskar mRNA is mislocalized to the anterior pole. Consistent
with the mislocalization of oskar mRNA, a fraction of the VASA protein
and nanos mRNA are also mislocalized to the anterior pole of bullwinkle
embryos. Mislocalization of nanos mRNA to the anterior is dependent on
functional VASA protein. Although the mirror-image segmentation defects
appear to result from the action of the posterior group genes, germ cells
are not formed at the anterior pole. The bicaudal phenotype is also germ-line
dependent for bullwinkle. We suspect that BULLWINKLE interacts with the
cytoskeleton and extracellular matrix and is necessary for gene product
localization and cell migration during oogenesis after stage 10a.
Nature 375 (6533): 654-658 (1995)
Polarization of both major body axes in Drosophila by gurken-torpedo
signalling.
Gonzalez-Reyes A, Elliott H, St Johnston D
Wellcome/CRC Institute, University of Cambridge, UK.
Anterior-posterior polarity in Drosophila arises from the movement of the
oocyte to the posterior of the egg chamber, and the subsequent acquisition
of posterior fate by the adjacent somatic follicle cells. We demonstrate
that gurken is necessary in the oocyte and torpedo/DER in the follicle
cells for the induction of posterior fate. As the gurken-torpedo/DER pathway
also establishes dorsoventral polarity later in oogenesis, Drosophila uses
the same germline to soma signalling pathway to determine both embryonic
axes.
Cell 81 (6): 967-978 (1995)
cornichon and the EGF receptor signaling process are necessary for
both anterior-posterior and dorsal-ventral pattern formation in Drosophila.
Roth S, Neuman-Silberberg FS, Barcelo G, Schupbach T
Department of Molecular Biology, Howard Hughes Medical Institute, Princeton
University, New Jersey 08544, USA.
In Drosophila, the dorsal-ventral polarity of the egg chamber depends on
the localization of the oocyte nucleus and the gurken RNA to the dorsal-anterior
corner of the oocyte. Gurken protein presumably acts as a ligand for the
Drosophila EGF receptor (torpedo/DER) expressed in the somatic follicle
cells surrounding the oocyte. cornichon is a gene required in the germline
for dorsal-ventral signaling. cornichon, gurken, and torpedo also function
in an earlier signaling event that establishes posterior follicle cell
fates and specifies the anterior-posterior polarity of the egg chamber.
Mutations in all three genes prevent the formation of a correctly polarized
microtubule cytoskeleton required for proper localization of the anterior
and posterior determinants bicoid and oskar and for the asymmetric positioning
of the oocyte nucleus.
Mech Dev 51 (2-3): 183-192 (1995)
The role of fs(1)K10 in the localization of the mRNA of the TGF alpha
homolog gurken within the Drosophila oocyte.
Serano TL, Karlin-McGinness M, Cohen RS
Department of Biochemistry, University of Kansas, Lawrence 66045, USA.
A critical step in Drosophila dorsoventral patterning is the movement of
gurken mRNA from the anterior cortex of the oocyte to the oocyte's anterodorsal
corner at stage 8 of oogenesis. Such movement is dependent on fs(1)K10.
It has been proposed that fs(1)K10 mediates gurken mRNA movement by down-regulating
gurken mRNA levels, thus ensuring that gurken mRNA does not saturate its
receptors located in the oocyte's anterodorsal corner. In contradiction
to this model, we show here--both genetically and immunocytochemically--that
GRK protein levels are lower in the anterodorsal region of fs(1)K10 mutant
oocytes than in the anterodorsal region of fs(1)K10+ oocytes. From this
and other data, we propose a more direct role for fs(1)K10 in the gurken
mRNA localization process.
Annu Rev Genet 29: 371-399 (1995)
Signaling pathways that establish the dorsal-ventral pattern of the
Drosophila embryo.
Morisato D, Anderson KV
Department of Biological Chemistry and Molecular Pharmacology, Harvard
Medical School, Boston, Massachusetts 02115, USA.
The dorsal-ventral pattern of the Drosophila embryo is established by three
sequential signaling pathways. Each pathway transmits spatial information
by localizing the activity of an extracellular signal, which acts as a
ligand for a broadly distributed transmembrane receptor. The components
of the first two pathways are encoded by maternal effect genes, while the
third pathway is specified by genes expressed in the zygote. During oogenesis,
the oocyte transmits a signal to the surrounding follicle cells by the
gurken-torpedo pathway. After fertilization, the initial asymmetry of the
egg chamber is used by the spatzle-Toll pathway to generate within the
embryo a nuclear gradient of the transcription factor Dorsal, which regulates
the regional expression of a set of zygotic genes. On the dorsal side of
the embryo, the decapentaplegic-punt/thick veins pathway then establishes
patterning of the amnioserosa and dorsal ectoderm. Each pathway uses a
distinct strategy to achieve spatial localization of signaling activity.
Genes Dev 8 (24): 2986-2995 (1994)
RNA localization along the anteroposterior axis of the Drosophila oocyte
requires PKA-mediated signal transduction to direct normal microtubule
organization.
Lane ME, Kalderon D
Department of Biological Sciences, Columbia University, New York, New York
10027.
Microtubule polarity has been implicated as the basis for polarized localization
of morphogenetic determinants that specify the anteroposterior axis in
Drosophila oocytes. We describe mutation affecting Protein Kinase A (PKA)
that act in the germ line to disrupt both microtubule distribution and
RNA localization along this axis. In normal oocytes, the site of microtubule
nucleation shifts from posterior to anterior immediately prior to polarized
localization of bicoid and oskar RNAs. In PKA-deficient oocytes, posterior
microtubules are present during this transition, oskar RNA fails to accumulate
at the posterior, and bicoid RNA accumulates at both ends of the oocyte.
Similar RNA mislocalization patterns previously reported for Notch and
Delta mutants suggest that PKA transduces a signal for microtubule reorganization
that is sent by posteriorly located follicle cells.
Science 266 (5185): 639-642 (1994)
Role of oocyte position in establishment of anterior-posterior polarity
in Drosophila.
Gonzalez-Reyes A, St Johnston D
Wellcome/CRC Institute, University of Cambridge, England.
The polarized microtubule cytoskeleton of the Drosophila oocyte directs
the localization of the maternal determinants which establish the anterior-posterior
(AP) axis of the embryo. Because the formation of this microtubule array
is dependent on signals from the follicle cells that surround the oocyte,
it has been proposed that AP polarity originates in the follicle cells.
Here it is shown that the movement of the oocyte to the posterior of the
egg chamber early in oogenesis determines AP polarity in the follicle cell
layer, and also in the oocyte. Moreover, the generation of AP asymmetry
requires signaling from the germ line to the soma and back again.
Curr Opin Genet Dev 4 (4): 502-507 (1994)
Dorsoventral patterning in Drosophila oogenesis.
Schupbach T, Roth S
Department of Molecular Biology, Princeton University, New Jersey 08544.
Dorsoventral polarity in the egg chamber of Drosophila involves the localization
of maternal gurken RNA to the dorsal side of the oocyte. The gurken protein
has homology to secreted growth factors and may bind to the torpedo/DER
receptor tyrosine kinase present on the adjacent follicle cells. This localized
signal from the oocyte to the follicle cells appears to initiate a cascade
of events leading to dorsal follicle cell differentiation, and delimiting
and orienting the future dorsoventral axis of the embryo.
Development 120 (5): 1233-1242 (1994)
Null alleles reveal novel requirements for Bic-D during Drosophila
oogenesis and zygotic development.
Ran B, Bopp R, Suter B
Department of Biology, McGill University, Montreal, PQ, Canada.
In the Drosophila ovary, the Bicaudal-D (Bic-D) gene is required for the
differentiation of one of 16 interconnected cystocyte sister cells into
an oocyte. A new class of Bic-Dnull alleles reveals a novel requirement
for Bic-D for zygotic viability. In the germ line, the null mutations show
that developmental processes that take place in germarial region 1, even
those that create asymmetry, are independent of Bic-D function. Bic-D is
then required to establish oocyte identity in one cystocyte and is essential,
not only for the oocyte-specific accumulation of all oocyte markers that
we have tested so far, but also for the posterior migration of the oocyte.
In addition, normal polarity amongst the nurse cells requires Bic-D, indicating
that the creation of different nurse cell identities may depend on oocyte
determination. Our results show that different processes in early oogenesis
require different amounts of Bic-D in a process-specific way and certain
later processes can proceed at low levels of Bic-D. This suggests that
the patterning of the female germ line and the development of an oocyte
depend on differential responses to a single activity that is capable of
initiating distinct oogenesis processes and can establish different cell
fates.
Curr Biol 4 (4): 289-300 (1994)
Transient posterior localization of a kinesin fusion protein reflects
anteroposterior polarity of the Drosophila oocyte.
Clark I, Giniger E, Ruohola-Baker H, Jan LY, Jan YN
Howard Hughes Medical Institute, University of California at San Francisco
94143-0724.
BACKGROUND: During oogenesis in Drosophila, determinants that will dictate
abdomen and germline formation are localized to the 'polar plasm' in the
posterior of the oocyte. Assembly of the polar plasm involves the sequential
localization of several messenger RNAs and proteins to the posterior of
the oocyte, beginning with the localization of oskar mRNA and Staufen protein
during stages 8 and 9 of oogenesis. The mechanism by which these two early
components accumulate at the posterior is not known. We have investigated
whether directed transport along microtubules could be used to accomplish
this localization. RESULTS: We have made a fusion protein composed of the
bacterial beta-galactosidase enzyme as a reporter, joined to part of the
plus-end-directed microtubule motor, kinesin, and have found that the fusion
protein transiently localizes to the posterior of the oocyte during stages
8 and 9 of oogenesis. Treatment with the microtubule-depolymerizing agent
colchicine prevents both the localization of the fusion protein and the
posterior transport of oskar mRNA and Staufen protein. Furthermore, the
fusion protein localizes normally in oocytes mutant for either oskar and
staufen, but not in other mutants in which oskar mRNA and Staufen protein
are mislocalized. CONCLUSIONS: Association with a plus-end-directed microtubule
motor can promote posterior localization of a reporter protein during oogenesis.
The genetic requirements for this localization and its sensitivity to colchicine,
both of which are shared with the posterior transport of oskar mRNA and
Staufen protein, suggest that similar mechanism may function in both processes.
Trends Genet 10 (3): 89-94 (1994)
The role of gene cassettes in axis formation during Drosophila oogenesis.
Ruohola-Baker H, Jan LY, Jan YN
Howard Hughes Medical Institute, University of California, San Francisco
94143-0724.
Establishment of the anteroposterior and dorsoventral axes of the fly originates
during oogenesis and relies on signaling between the oocyte and the surrounding
somatic follicle cells. Some genes originally identified as playing a role
in signaling during embryonic development also mediate cell-cell communication
during oogenesis. These genes have previously been grouped on the basis
of their functions during embryogenesis, and this classification is largely
maintained in oogenesis. The EGF receptor, the transmembrane protein rhomboid
and proteins in the ras signal transduction pathway are required to initiate
dorsoventral polarity, whereas the products of the neurogenic genes Notch
and Delta are necessary for formation of the anteroposterior axis in the
oocyte.
Genes Dev 8 (5): 598-613 (1994)
The Drosophila orb RNA-binding protein is required for the formation
of the egg chamber and establishment of polarity.
Lantz V, Chang JS, Horabin JI, Bopp D, Schedl P
Department of Molecular Biology, Moffett Laboratory, Princeton University,
New Jersey 08544.
The orb gene of Drosophila encodes sex-specific germ-line proteins that
contain two RRM-type RNA-binding domains. Here we report the distribution
of Orb protein in wild-type, tumorous, and orb mutant ovaries. The wild-type
distribution of Orb protein during oogenesis resembles that of its RNA,
preferentially accumulating in the cytoplasm of the developing oocyte shortly
after the formation of the 16-cell cyst. As anticipated from its germ-line
expression, mutations in orb lead to female sterility. Analysis of the
effect of orb mutants on the distribution of RNAs known to be required
for oocyte differentiation and polarity suggests that orb functions in
RNA localization at multiple points during oogenesis. In addition, phenotypic
characterization of the orb mutants indicates that the gene is required
early in oogenesis for formation of the 16-cell cyst. It then functions
in the differentiation of the oocyte and is required for the three-dimensional
reorganization of the germ cells in the cyst as well as for the establishment
of normal germ-line-soma interactions in the egg chamber.
Cell 75 (1): 165-174 (1993)
The Drosophila dorsoventral patterning gene gurken produces a dorsally
localized RNA and encodes a TGF alpha-like protein.
Neuman-Silberberg FS, Schupbach T
Department of Molecular Biology, Princeton University, New Jersey 08544.
Cell-cell interactions in the Drosophila ovary play a crucial role in the
establishment of dorsoventral polarity of both the egg shell and the future
embryo. Torpedo/DER (top/DER), a homolog of the vertebrate epidermal growth
factor receptor, is required for this signaling process in the somatic
cells of the ovary. In contrast, gurken (grk), which also functions in
this pathway, is required in the germline. We cloned the grk gene and found
that it encodes a TGF alpha-like protein. Grk is, therefore, likely to
be a ligand of top/DER, activating the receptor during oogenesis. During
oogenesis, the grk transcript becomes asymmetrically localized to the dorsal
corner of the oocyte. We propose that the dorsal localization of grk RNA
results in a spatially restricted ligand that asymmetrically activates
the receptor.
Ann Genet 36 (1): 5-15 (1993)
Determination of the dorso-ventral polarity of the Drosophila embryo
Mohier E
CNRS, Institut Jacques-Monod, Paris, France.
Embryonic pattern formation has been studied extensively in many organisms.
In Drosophila, the powerful combination of genetics cytoplasm transplantation
experiments, as well as recent molecular data, have helped to elucidate
the mechanisms responsible for the establishment of embryonic polarity.
A small number of genes, most of them maternally expressed, are involved
in this process and participate in four independent systems--three for
the antero-posterior axis (A/P) and one for dorsoventral axis (D/V)--which
define various embryonic territories by specifically localized cues. This
review concerns the definition of the dorsoventral polarity responsible
for the establishment of the germ layers of the embryo. Dorsoventral development
is regulated by a single group of maternally expressed genes: the "dorsal
group" of genes. It includes 11 genes, the loss of function of any of which
results in a dorsalized development, whereas mutation of the 12th gene,
cactus, results in a ventralized development. These genes are arranged
according to a functional hierarchy, and have been shown to cooperate in
the formation of a graded nuclear concentration of the dorsal gene product.
The dorsal product corresponds to the dorsoventral morphogen and is homologous
to the transcription factor NF-kappa B. Among the 11 genes of the dorsal
group, 3 are required in the somatic line. This suggests the existence
of inductive signals originating during oogenesis from the follicle cells
that surround the developing oocyte. This somatically expressed spatial
information probably controls dorsoventral development by defining the
polarity of a signal transducing pathway that specifically activates the
nuclear uptake of the dorsal product. This model, highlights the importance
of the polarity of the egg chamber, and suggests that it is the oocyte
nucleus due to its asymmetrical localization, that determines the dorsoventral
pattern formation of the embryo.
Development 116 (1): 177-192 (1992)
The neurogenic locus brainiac cooperates with the Drosophila EGF receptor
to establish the ovarian follicle and to determine its dorsal-ventral polarity.
Goode S, Wright D, Mahowald AP
University of Chicago, Department of Molecular Genetics and Cell Biology,
Cummings Life Science Center, IL 60637.
We have characterized the function of a new neurogenic locus, brainiac
(brn), during oogenesis. Homozygous brn females lay eggs with fused dorsal
appendages, a phenotype associated with torpedo (top) alleles of the Drosophila
EGF receptor (DER) locus. By constructing double mutant females for both
brn and top, we have found that brn is required for determining the dorsal-ventral
polarity of the ovarian follicle. However, embryos from mature brn eggs
develop a neurogenic phenotype which can be zygotically rescued if a wild-type
sperm fertilizes the egg. This is the first instance of a Drosophila gene
required for determination of dorsal-ventral follicle cell fates that is
not required for determination of embryonic dorsal-ventral cell fates.
The temperature-sensitive period for brn dorsal-ventral patterning begins
at the inception of vitellogenesis. The interaction between brn and DER
is also required for at least two earlier follicle cell activities which
are necessary to establish the ovarian follicle. Prefollicular cells fail
to migrate between each oocyte/nurse cell complex, resulting in follicles
with multiple sets of oocytes and nurse cells. brn and DER function is
also required for establishing and/or maintaining a continuous follicular
epithelium around each oocyte/nurse cell complex. These brn functions as
well as the brn requirement for determination of dorsal-ventral polarity
appear to be genetically separable functions of the brn locus. Genetic
mosaic experiments show that brn is required in the germline during these
processes whereas the DER is required in the follicle cells. We propose
that brn may be part of a germline signaling pathway differentially regulating
successive DER-dependent follicle cell activities of migration, division
and/or adhesion and determination during oogenesis. These experiments indicate
that brn is required in both tyrosine kinase and neurogenic intercellular
signaling pathways. Moreover, the functions of brn in oogenesis are distinct
from those of Notch and Delta, two other neurogenic loci that are known
to be required for follicular development.
In Vivo 5 (5): 443-456 (1991)
Models of pattern formation in insect oocytes.
Kunkel JG
Zoology Department, University of Massachussets, Amherst 01003.
Pattern formation in early insect development is dominated by coordination
of the germ lines polarity with the polarity of the follicle cell layer.
The production of an elaborate protective chorion, covering the ovulated
oocyte, has made establishing parallel polarity of germ line and soma absolutely
essential. Genetics and molecular biology, particularly on Drosophila melanogaster,
have identified numerous signals passed from follicle cell to oocyte and
vice versa. The physiological basis of this communication is beginning
to be established with the identification of several membrane receptors
and potential signal transduction steps. The contributions of three physiological
models of pattern formation are discussed as they relate to the growing
genetic model. Evidence for and against ionic currents as factors in polarity
determinations is particularly emphasized.
Development 107 Suppl: 169-180 (1989)
Models for positional signalling with application to the dorsoventral
patterning of insects and segregation into different cell types.
Meinhardt H
Max-Planck-Institut fur Entwicklungsbiologie, Tubingen, FRG.
Models of pattern formation and possible molecular realizations are discussed
and compared with recent experimental observations. In application to the
dorsoventral patterning of insects, it is shown that a superposition of
two pattern-forming reactions is required. The first system generates the
overall dorsoventral polarity of the oocyte, the second generates the positional
information proper with a stripe-like region of high concentration along
the ventral side of the embryo. A single reaction would be insufficient
since the two reactions require different parameters. The model accounts
for the orientation of the DV axes of the oocytes in the ovary of Musca
domestica and Sarcophaga, independent of the DV axis of the mother, for
the formation of several ventral furrows in the absence of the primary
gurken/torpedo system in Drosophila, as well as for the good size regulation
of the dorsoventral axis as observed in some insect species. Segregation
of a homogeneous cell population into different cell types requires autocatalytic
processes that saturate at relatively low concentrations and nondiffusible
substances responsible for the autocatalytic feed-back loops. Thus, these
loops can be realized directly on the gene level via their gene products,
for instance, by the mutual repression of two genes. A balance of the two
cell types is achieved by a long-ranging substance interfering with the
self-enhancing process. This substance is expected to have a more or less
homogeneous distribution. This model accounts for the reestablishment of
the correct proportion after an experimental interference and the change
of determination after transplantation. Applications to the segregation
of pre-stalk and prespore cells in Dictyostelium and of neuroblast cells
from the ventral ectoderm in Drosophila are provided.
Development 107 Suppl: 13-19 (1989)
Multiple steps in the localization of bicoid RNA to the anterior pole
of the Drosophila oocyte.
St Johnston D, Driever W, Berleth T, Richstein S, Nusslein-Volhard
C
Max Planck Institut fur Entwicklungsbiologie, Abteilung Genetik, Tubingen,
FRG.
The anterior region of the Drosophila embryonic pattern is determined by
a gradient of the bicoid (bcd) protein. The correct formation of this gradient
requires the localization of bcd RNA to the anterior pole of the egg. Here
we use a wholemount in situ technique to examine the process of bcd RNA
localization during oogenesis and embryogenesis. While bcd protein becomes
distributed in a gradient that extends throughout the anterior two thirds
of the early embryo, bcd RNA remains restricted to a much smaller region
at the anterior pole. The difference between these distributions indicates
that the shape of the protein gradient must depend to some extent on the
posterior movement of the protein after it has been synthesized. Four distinct
phases of bcd RNA localization can be distinguished during oogenesis. Between
stages 6 and 9 of oogenesis, the RNA accumulates in a ring at the anterior
end of the oocyte. During the second phase, in stage 9-10a follicles, the
RNA also localizes to the apical regions of the nurse cells, demonstrating
that the nurse cells possess an intrinsic polarity. As the nurse cells
contract during stages 10b-11, all of the bcd RNA becomes localized to
the cortex at the anterior end of the oocyte. During a final phase that
must occur between stage 12 of oogenesis and egg deposition, the RNA becomes
localized to a spherical region that occupies a slightly dorsal position
at the anterior pole.
Nature 335 (6185): 68-70 (1988)
Drosophila nurse cells produce a posterior signal required for embryonic
segmentation and polarity.
Sander K, Lehmann R
Biol. Institut I (Zoologie), Freiburg, FRG.
The segmental pattern of insect embryos depends on influences from morphogenetic
centres near each of the egg poles. In Drosophila, maternal effect mutations
are known that impair the normal function of each centre. Injection of
wild-type cytoplasm into mutant eggs has revealed that morphogenetic signals
localized at the anterior and posterior pole of eggs can be transplanted.
We show here that these activities can also be detected during oogenesis.
Posterior activity can be recovered at an early stage (stage 10, ref. 5)
from the oocyte-nurse cell complex, but anterior activity can only be detected
in the mature oocytes (stage 14). We conclude that the bicoid-dependent
anterior signal, although produced by the nurse cells, does not become
active before it is localized to the anterior egg pole, whereas posterior
activity can be detected in the nurse cells before, and therefore independently
of, its localization to the posterior egg pole.
Biol Reprod 32 (1): 27-42 (1985)
Roles of cell-to-cell communication in development.
Schultz RM
Possible roles of cell-to-cell communication mediated by intercellular
bridges and gap junctions in development of the female gamete and embryo
are discussed. Synchronization of cell cycle events is presumably a role
for intercellular bridges between germ cells. The follicle of the Cecropia
moth reveals that an electrical polarity exists between nurse cells and
oocytes which are connected by intercellular bridges and this polarity
may generate differences that result in differentiation of the oogonia
to become either the oocyte or nurse cells. Gap junction-mediated transfer
of cyclic AMP, made in response to gonadotropin stimulation, between granulosa
cells is discussed as a mechanism that allows cells within a tissue to
respond to an external stimulus even though all cells in that tissue may
not be exposed to the stimulus. A nutritional role for heterologous cell
communication between follicle cells and the oocyte in oocyte growth is
presented as an example of how gap junction-mediated communication can
allow one cell type to influence the behavior of another cell type. During
development, a restriction in communication between differentiating cells
is frequently observed. Examples of this phenomenon in a mammal and an
insect are presented.