FB2026_02 , released June 18, 2026
Allele: Dmel\MED311
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General Information
Symbol
Dmel\MED311
Species
D. melanogaster
Name
FlyBase ID
FBal0239038
Feature type
allele
Associated gene
Associated Insertion(s)
Carried in Construct
Key Links
Genomic Maps

Mutagen
    Nature of the Allele
    Mutagen
    Progenitor genotype
    Associated Insertion(s)
    Cytology
    Description

    P{lacW} insertion in the 5' UTR of the MED31-RA isoform. The insertion is also exactly after the first splice donor site of intron I of the MED31-RB isoform.

    Allele components
    Component
    Use(s)
    Inserted element
    Encoded product / tool
    Mutations Mapped to the Genome
    Curation Data
    Variant Molecular Consequences
    Associated Sequence Data
    DNA sequence
    Protein sequence
     
    Expression Data
    Reporter Expression
    Additional Information
    Statement
    Reference
     
    Marker for
    Reflects expression of
    Reporter construct used in assay
    Human Disease Associations
    Disease Ontology (DO) Annotations
    Models Based on Experimental Evidence ( 0 )
    Disease
    Evidence
    References
    Modifiers Based on Experimental Evidence ( 0 )
    Disease
    Interaction
    References
    Comments on Models/Modifiers Based on Experimental Evidence ( 0 )
     
    Disease-implicated variant(s)
     
    Phenotypic Data
    Phenotypic Class
    Phenotype Manifest In
    Detailed Description
    Statement
    Reference

    Homozygous females show reduced fecundity, laying 7.4 +/- 1.5 eggs/20 hours (compared to 46.0 +/- 3.3 eggs/20 hours for wild-type females). MED311/Df(3R)Z1 females also show reduced fecundity, laying 3.2 +/- 0.4 eggs/20 hours.

    Only 2.1% of embryos laid by homozygous females mated to wild-type males hatch.

    Only 3.2% of embryos laid by MED311/Df(3R)Z1 females mated to wild-type males hatch.

    91.6% of embryos laid by MED311/MED3121 females mated to wild-type males hatch.

    The majority of embryos laid by homozygous or MED311/Df(3R)Z1 females (independent of paternal genotype) show severe morphological defects beyond stage 8.

    Embryos derived from homozygous females mated to wild-type males reach the cellular blastoderm stage, but begin to display severe defects upon gastrulation. The proctodeal invagination, transverse furrow, stomodeal invagination and the cephalic furrow do form in the mutant embryos. However, the mitotic domains are missing or completely mislocalised in the mutant embryos and coincide with abnormal morphology. The formation of the posterior pole cells appears unaffected in the mutant embryos, but shortly after their formation, cells at the anterior and posterior pole start to delaminate toward the interior of the embryo. Abnormal cell ingression is seen at the anterior-dorsal region of the embryo. Cells associated with the migrating polar plate behave abnormally, resulting in severe deformations at the posterior-dorsal region of the embryo. During later stages, abnormal migration and degeneration at the poles results in cell loss.

    A small proportion of embryos laid by homozygous females hatch, and some of these larvae progress through development and produce adult escapers. 33.7% of adult escapers derived from homozygous females mated to wild-type males have abdominal segmentation defects and 45.6% of adult escapers derived from homozygous females mated to homozygous males have abdominal segmentation defects. Defects in both sexes include incomplete tergite separation and additional tergites (13.4%), distinct patches of pigment in the abdominal epidermis (14.3%) and abnormally positioned sternites. Haltere development is disrupted in 10.6% of cases.

    MED311/Df(3R)Z1 and MED311/MED311 adults derived from heterozygous parents do not develop significant abdominal defects.

    External Data
    Interactions
    Show genetic interaction network for Enhancers & Suppressors
    Phenotypic Class
    NOT Enhancer of
    Statement
    Reference

    MED311/MED31[+] is a non-enhancer of visible | maternal effect | dominant phenotype of skdL7062

    Phenotype Manifest In
    Enhanced by
    Statement
    Reference

    MED311 has adult epidermis | maternal effect phenotype, enhanceable by skdL7062/skd[+]

    NOT Enhancer of
    Statement
    Reference

    MED311/MED31[+] is a non-enhancer of adult abdomen | maternal effect phenotype of skdL7062

    Additional Comments
    Genetic Interactions
    Statement
    Reference

    When MED311/MED311 females are crossed to skdL7062/+ males, 54.7% of the MED311/skdL7062 adult progeny have abdominal defects, indicating that zygotic skdL7062 enhances the MED311 phenotype.

    No increase in abdominal segmentation defects is seen in the adult progeny of MED311/skdL7062 females compared to the defects of the progeny of skdL7062/+ females, indicating that MED311 is not an enhancer of skdL7062 when maternally supplied.

    Xenogenetic Interactions
    Statement
    Reference
    Complementation and Rescue Data
    Partially rescued by

    MED311 is partially rescued by MED31tBa

    Comments
    Images (0)
    Mutant
    Wild-type
    Stocks (0)
    Notes on Origin
    Discoverer
    External Crossreferences and Linkouts ( 0 )
    Synonyms and Secondary IDs (2)
    Reported As
    Symbol Synonym
    MED311
    Name Synonyms
    Secondary FlyBase IDs
      References (1)