- Tools
- Downloads
- Links
- Community
- About
- Help
FB2026_01
,
released March 12, 2026
male sterile (with peloPB60)
pelo1 mutant adults display resistance (higher survival rate) to Drosophila C Virus infection compared to controls.
The germaria of pelo1 females have a lower number of germline stem cells (GSCs) that heterozygous controls; 7-day-old pelo1 germaria have an average of 0.47 GSCs (vs. 2.4 GSCs in controls) with over half of them containing no GSC. pelo1 germaria that do have 2 GSCs are small and contain very few germline cysts. No dying GSCs can be detected in pelo1 germaria but dying cysts are observed. A lower amount of pelo1 GSCs incorporate BrdU compared to controls, showing that GSC division is reduced. The self-renewal of GSCs is also affected in pelo1 mutants as 55% of GSCs are maintained over a 3 week period in wild-type controls while over 97% of GSCs are lost over the same period in the mutants. pelo1/Df(2L)s1402 females also exhibit a low number of GSCs. The formation and survival of somatic cells in the germarium is not affected in pelo1 mutants. Mutant follicle cell clones exhibit a very minor phenotype, appearing slightly thinner than wild-type follicle cells. pelo1 females are partially fertile after eclosion but quickly lose their fertility. This is reflected by the presence of some mature eggs in 2-day-old mutant ovaries, while 7-day-old ovaries rarely contain egg chambers that have progressed beyond stage 9. The early stage egg chambers, which contain an oocyte, exhibit condensed nurse cell DNA, suggesting that they are undergoing apoptosis, and are often smaller than wild-type egg chambers. pelo1 germline cysts also fail to grow to a normal size and become apoptotic.
Homozygotes are fully viable at 18oC and 25oC, but have reduced viability in crowded conditions. Homozygous males show cell cycle arrest in spermatocytes just before, or very early in, the first meiotic cell division. Other aspects of spermatogenesis continue normally, resulting in 4N spermatids. Phenotype closely resembles that of twe1. Spindle formation and nuclear envelope breakdown fail, but chromosome condensation proceeds normally. In some homozygous adults, eyes are roughened, with disordered ommatidial arrays and bristles. Eyes tend to be smaller than in wild-type siblings. Homozygous females have reduced fertility, and ovaries are reduced in size. The mitotic zone of the germarium appears disorganized and often contains degenerating cells.
Meiosis does not occur, abnormally large nebenkern form in later spermatocytes. Semi-lethal.
cold-sensitive. female-sterile. Meiosis does not occur; abnormally large Nebenkern forms in late spermatocytes.
pelo1/peloPB60 has female sterile phenotype, suppressible | partially by Scer\GAL4VP16.nanos.UTR/RpS30UASp.cYa
pelo1/peloPB60 has male sterile phenotype, suppressible by Mmus\PeloUASp.cYa/Scer\GAL4αTub84B.PL
pelo1/peloPB60 has male sterile phenotype, non-suppressible by Mmus\PeloUASp.cYa/Scer\GAL4VP16.nanos.UTR
pelo1 has decreased cell number | oogenesis phenotype, non-suppressible by bamΔ86
pelo[+]/pelo1 is a suppressor | partially of neoplasia phenotype of Scer\GAL4C587, dppUAS.cNa
pelo1/peloPB60 has testis phenotype, suppressible | partially by Mmus\PeloUASp.cYa/Scer\GAL4αTub84B.PL
pelo[+]/pelo1 is a suppressor | partially of female germline stem cell phenotype of Scer\GAL4C587, dppUAS.cNa
pelo1 is a suppressor of female germline stem cell phenotype of bamΔ86
pelo[+]/pelo1 is a non-suppressor of female germline stem cell phenotype of bamΔ86
The near complete sterility (minimal number of laid eggs, very low hatching rate) of pelo1/peloPB60 transheterozygous females can be partially rescued by expression of RpS30Scer\UAS.P\T.cYa under the control of Scer\GAL4nos.UTR.T:Hsim\VP16 in the mutant background.
In pelo1;bamΔ86 double mutant germaria, germ cells are able to differentiate as cystocytes can form. This is evidenced by branched fusomes, although the morphology of these fusomes is abnormal. However, some germ cells remain undifferentiated, as abnormally enlarged spectrosomes persist. Germ cell differentiation is not rescued when bamΔ86 homozygous mutants are pelo1/+; these germaria also show the rapid loss of GSCs observed in pelo1 germaria. When dppScer\UAS.cNa is expressed under the control of Scer\GAL4C587 in a pelo1/+ background, 64% of ovarioles no longer show the stem cell tumour phenotype seen when dppScer\UAS.cNa is expressed in a wild-type background. These ovarioles contain differentiated germline cysts, developing egg chambers and mature eggs. When dppScer\UAS.cNa is expressed in a pelo1 homozygous background, the tumour phenotype is further suppressed.
The spermatogenesis defects but not male sterility characteristic for pelo1/peloPB60 transheterozygous flies can be partially rescued by expression of Mmus\PeloScer\UAS.P\T.cYa under the control of Scer\GAL4nos.UTR.T:Hsim\VP16 while the Scer\GAL4αTub84B.PL-driven expression restores male fertility to near wild-type level.
pelo1/peloPB60 is rescued by peloUASp.cXa/Scer\GAL4VP16.nanos.UTR
pelo1/peloPB60 is rescued by peloUASp.cXa/Scer\GAL4αTub84B.PL
pelo1 is rescued by peloUASp.cXa/Scer\GAL4VP16.nanos.UTR
pelo1 is rescued by Scer\GAL4VP16.nanos.UTR/pelonls.UASp.Tag:FLAG,Tag:MYC
pelo1 is rescued by peloUASp.Tag:FLAG,Tag:MYC/Scer\GAL4VP16.nanos.UTR
pelo1/peloPB60 is partially rescued by Scer\GAL4VP16.nanos.UTR/peloP210A.UASp
pelo1/peloPB60 is partially rescued by peloUASp.cXa/Scer\GAL4VP16.nanos.UTR
pelo1 is partially rescued by peloUASp.cXa
pelo1 is partially rescued by peloUASp.cXa/Scer\GAL4C587
pelo1 is not rescued by pelonls.UASp.Tag:FLAG,Tag:MYC
pelo1 is not rescued by Scer\GAL4C587/pelonls.UASp.Tag:FLAG,Tag:MYC
Expressing peloUASp.cXa under the control of Scer\GAL4VP16.nos.UTR fully rescues the male sterility and spermatogenesis defects (male germline stem cell number, individualization complex formation and spermatid nuclei elongation defects) observed in peloPB60/pelo1 transheterozygotes. Expressing peloP210A.UASp under the control of Scer\GAL4VP16.nos.UTR, however, fails to rescue the male sterility and individualization complex formation defects, and only partially rescues the male germline stem cell number and spermatid nuclei elongation defects.
The near complete sterility (minimal number of laid eggs, very low hatching rate) of pelo1/peloPB60 transheterozygous females can be partially rescued by expression of peloScer\UAS.P\T.cXa under the control of Scer\GAL4nos.UTR.T:Hsim\VP16 in the mutant background. Expression under the Scer\GAL4nos.UTR.T:Hsim\VP16 driver rescues the spermatogenesis defects (no individualization complexes and waste bags) as well as the male sterility, which can also bes rescued by Scer\GAL4αTub84B.PL-driven expression.
The GSC loss phenotype in pelo1 females is partially recued by leaky expression of the peloScer\UAS.P\T.cXa transgene without a driver; expression of Scer\GAL4C587 in the somatic cells of the germarium confers very limited extra rescue compared to that conferred by the transgene alone.
A. Spradling.
Complements: Pka-C101272. Complements: ms(2)30C07822.
P\TΔ2-3-induced reversion correlates precise excision of the P{PZ} with reversion of the pelo1 mutant phenotype. Phenotype of pelo1/Df(2L)30A-C is indistinguishable from that of pelo1 homozygotes.