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Allele Dmel\shot^HG25

General Information
Symbol	Dmel\shotHG25	Species	D. melanogaster
Name		FlyBase ID	FBal0095203
Feature type	allele	Associated gene	Dmel\shot
Allele class
Mutagen
Recent Updates
Description	What does this section display? This section contains items that were added to this record for each release. It currently only tracks new links between this FlyBase report and other FlyBase data classes (e.g. genes, references, stocks) or controlled vocabulary terms (e.g. GO, anatomy terms). What does this section not display? This section does not currently display links that were removed or gene model changes.
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FB2013_03
FB2013_02
All updates	Click here to see a list of all updates to this record from FB2010_08 and on.
Nature of the Allele
Allele class
Mutagen
Mutations Mapped to the Genome
Type Location Additional Notes References
Associated Sequence Data
DDBJ / EMBL / GenBank	DNA sequence Protein sequence Name
UniProtKB/Swiss-Prot
UniProtKB/TrEMBL
Progenitor genotype
Nature of the lesion	Statement Reference
Cytology
Phenotypic Data
Phenotypic Class
	lethal | embryonic stage | recessive (Prokop et al., 1998) neuroanatomy defective | embryonic stage (with shot91k) (Prokop et al., 1998) paralytic | recessive (Prokop et al., 1998)
Phenotype Manifest In
	embryonic/first instar larval cuticle (Prokop et al., 1998) embryonic/larval somatic muscle (Prokop et al., 1998) muscle attachment site | embryonic stage (Prokop et al., 1998) neuromuscular junction | embryonic stage (Prokop et al., 1998) synapse & neuromuscular junction (Lohr et al., 2002)
Detailed Description
	Statement Reference shotHG25 mutants show strong reduction of output synapses at the NMJ, while this phenotype is not seen in the CNS. (Lohr et al., 2002) Homozygous and hemizygous embryos show a paralytic phenotype. Neuromuscular junctions occupy far less surface of their respective muscles, their branches are reduced in length and boutons appear reduced in number and size in hemizygous and shotHG25/shot91k embryos compared to wild-type. Peripheral nerves can form correctly in shot91k/shotHG25 embryos. The short SNb-branch has a tendency to stall in these embryos. shot91k/shotHG25 embryos do not show any obvious defects in muscle patterning at stage 16. However, at stage 17, severe detachment of the muscles from the cuticle is seen, although the muscles remain attached to each other. (Prokop et al., 1998)
External Data
Linkouts
Interactions
Phenotypic Class
Phenotype Manifest In
Additional Comments
Genetic Interactions
Statement Reference
Xenogenetic Interactions
Statement Reference
Complementation & Rescue Data
Fails to complement	shot91k (Prokop et al., 1998) shotel3 (Prokop et al., 1998) shotk03405 (Prokop et al., 1998) shotSF20 (Prokop et al., 1998) shotV168 (Prokop et al., 1998)
Comments
Stocks ( 0 )
Notes on Origin
Discoverer
	Selected as: wb allele in screen over wbSF20. (Prokop et al., 1998)
External Crossreferences & Linkouts
Other Crossreferences
Linkouts
Synonyms & Secondary IDs ( 2 )
Reported As
Symbol Synonym	kakHG25 (Lohr et al., 2002, ) shotHG25
Name Synonym
Secondary FlyBase IDs
References ( 2 )
Research paper	Lohr et al., 2002, J. Neurosci. 22(23): 10357--10367 Compartmentalization of central neurons in Drosophila: a new strategy of mosaic analysis reveals localization of presynaptic sites to specific segments of neurites. [FBrf0152141] Prokop et al., 1998, J. Cell Biol. 143(5): 1283--1294 The kakapo mutation affects terminal arborization and central dendritic sprouting of Drosophila motorneurons. [FBrf0105910]