FB2026_01 , released March 12, 2026
FB2026_01 , released March 12, 2026
Allele: Dmel\parkSE.UAS
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General Information
Symbol
Dmel\parkSE.UAS
Species
D. melanogaster
Name
FlyBase ID
FBal0302844
Feature type
allele
Associated gene
Dmel\park
Associated Insertion(s)
Carried in Construct
P{UAS-park.SE}
Also Known As
UAS-dParkin S94E
Key Links
Transgenic product class
missense_variant
(Shiba-Fukushima et al., 2014)
polypeptide_post_translational_processing_variant
(Shiba-Fukushima et al., 2014)
Mutagen
Nature of the Allele
Transgenic product class
missense_variant
(Shiba-Fukushima et al., 2014)
polypeptide_post_translational_processing_variant
(Shiba-Fukushima et al., 2014)
Mutagen
in vitro construct
(Shiba-Fukushima et al., 2014)
Progenitor genotype
Carried in construct
P{UAS-park.SE}
Cytology
Description

UASt regulatory sequences drive expression of a phosphomimetic form of park in which the serine at amino acid 94 has been replaced by glutamic acid.

(Shiba-Fukushima et al., 2014)
Allele components
Component
Use(s)
Regulatory region(s)
UASt
Encoded product / tool
park
Mutations Mapped to the Genome
Curation Data
Type
Location
Additional Notes
References
Variant Molecular Consequences
Associated Sequence Data
DDBJ / EMBL / GenBank
DNA sequence
Protein sequence
 
UniProtKB/Swiss-Prot
    UniProtKB/TrEMBL
      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 ( 1 )
      Disease
      Evidence
      References
      model of  Parkinson's disease 6
      CEC
      (Liu et al., 2022)
      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

      Expression of parkSE.Scer\UAS in indirect flight muscles under the control of Scer\GAL4Mhc.PU results in over-fragmentation of mitochondria compared with controls. ATP content is reduced compared with controls in 40 day old flies.

      Expression of parkSE.Scer\UAS under the control of Scer\GAL4Mhc.PU enhances the decline in climbing ability seen in older flies. The flies have an abnormal wing posture even in young adult flies.

      Expression of parkScer\UAS.cSa under the control of Scer\GAL4ple.PU causes a reduction in the number of tubular mitochondria in the cell bodies of dopaminergic neurons in 5 day old flies compared to controls, resulting in a single large aggregate of mitochondria in each cell body. The mitochondria seen outside of the cell body are not seen.

      Flies expressing parkSE.Scer\UAS under the control of Scer\GAL4ple.PU exhibit reduced flying ability compared to controls.

      Expression of parkSE.Scer\UAS under the control of Scer\GAL4ple.PU results in loss of dopaminergic neurons in 5-day old flies.

      (Shiba-Fukushima et al., 2014)
      External Data
      Interactions
      Show genetic interaction network for Enhancers & Suppressors
      Phenotypic Class
      Suppressed by
      Statement
      Reference

      Scer\GAL4Mhc.PU, parkSE.UAS has visible phenotype, suppressible | partially by Scer\GAL4Mhc.PU

      (Shiba-Fukushima et al., 2014)
      NOT suppressed by
      Statement
      Reference

      Scer\GAL4ple.PU, parkSE.UAS has abnormal neuroanatomy phenotype, non-suppressible by Pink1B9

      (Shiba-Fukushima et al., 2014)
      Suppressor of
      Statement
      Reference

      parkSE.UAS/Scer\GAL4Mhc.PU is a suppressor of short lived phenotype of Pink1B9

      (Shiba-Fukushima et al., 2014)
      NOT Suppressor of
      Phenotype Manifest In
      Additional Comments
      Genetic Interactions
      Statement
      Reference

      Expression of Pink1dsRNA.Scer\UAS does not suppress the over-fragmentation of mitochondria seen when parkSE.Scer\UAS is expressed in indirect flight muscles under the control of Scer\GAL4Mhc.PU.

      Expression of parkSE.Scer\UAS suppresses the increase in mitochondrial length seen when Pink1dsRNA.Scer\UAS is expressed under control of Scer\GAL4Mhc.PU.

      Expression of parkSE.Scer\UAS under the control of Scer\GAL4Mhc.PU in a Pink1B9 mutant background results in reduced ATP levels compared to expression of parkSE.Scer\UAS or Pink1B9 alone.

      Expression of parkSE.Scer\UAS under the control of Scer\GAL4Mhc.PU fails to suppress the climbing defects seen in Pink1B9 mutant flies.

      Pink1B9 partially suppresses the abnormal wing posture seen in flies expressing parkSE.Scer\UAS under the control of Scer\GAL4Mhc.PU.

      Pink1B9 does not suppress the mitochondria defects seen when parkSE.Scer\UAS is expressed under the control of Scer\GAL4ple.PU.

      Pink1B9 does not suppress the dopaminergic neuron loss seen when parkSE.Scer\UAS is expressed under the control of Scer\GAL4ple.PU.

      (Shiba-Fukushima et al., 2014)
      Xenogenetic Interactions
      Statement
      Reference
      Complementation and Rescue Data
      Comments

      Expression of parkSE.Scer\UAS under the control of Scer\GAL4da.PU results in lethality, either in a parkΔ21/park1 or wild type mutant background.

      (Shiba-Fukushima et al., 2014)
      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
      parkSE.Scer\UAS
      parkSE.UAS
      Name Synonyms
      Secondary FlyBase IDs
        References (3)