Reference Report

Reference
Citation	Panz, M., Vitos-Faleato, J., Jendretzki, A., Heinisch, J.J., Paululat, A., Meyer, H. (2012). A novel role for the non-catalytic intracellular domain of Neprilysins in muscle physiology. Biol. Cell 104(9): 553--568. (Export to RIS)
FlyBase ID	FBrf0219388
Publication Type	Research paper
PubMed ID	22583317
PubMed Abstract	Neprilysins (Neps) are membrane-bound M13 endopeptidases responsible for the activation and/or inactivation of peptide signalling events on cell surfaces. By hydrolysing their respective substrates, mammalian Neps are crucial to the metabolism of numerous bioactive peptides, especially in the nervous, immune, cardiovascular and inflammatory systems. On the basis of their involvement in essential physiological processes, proteins of the Nep family constitute putative therapeutic agents as well as targets in different diseases, including Alzheimer's disease.We here demonstrate that overexpression of Neprilysin 4 (Nep4) in Drosophila melanogaster leads to a severe muscle degeneration phenotype. This phenotype is observed for overexpression of full-length Nep4 in somatic muscles and is accompanied by severely impaired movement of larvae and lethality in late larval development. On the contrary, down-regulation of expression caused only the latter two effects. By expressing several mutated and truncated forms of Nep4 in transgenic animals, we show that the intracellular domain is responsible for the observed phenotypes while catalytic activity of the enzyme was apparently dispensable. A yeast two-hybrid screen identified a yet uncharacterised carbohydrate kinase as a first interaction partner of the intracellular domain of Nep4.These data demonstrate that the physiological significance of Nep4 is not limited to its function as an active peptidase but that the enzyme's intracellular N-terminus is affecting muscle integrity, independent of the protein's enzymatic activity. To our knowledge, this is the first report of an intracellular Nep domain being involved in muscle integrity.
DOI	10.1111/boc.201100069
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Language of Publication	English
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Publication Type	Journal
Abbreviation	Biol. Cell
Title	Biology of the Cell
Publication Year	1981-
ISBN/ISSN	0248-4900
Data from Reference
Alleles (21)
	Avic\GFP^{hs.Stinger.T:nls-tra} Avic\GFP^{Nep4.meso.T:nls-tra} CG3534^GD5710 CG3534^KK102673 Nep1^EY21255 Nep4^A.T:Ivir\HA1 Nep4^{FExxH.Scer\UAS.A} Nep4^GD5655 Nep4^{HExxF.Scer\UAS.A} Nep4^{HQxxH.Scer\UAS.A} Nep4^KK104462 Nep4^Scer\UAS.A Nep4^Scer\UAS.B Nep4^{trunc.Scer\UAS.A} Scer\GAL4^Act5C.PI Scer\GAL4^elav.PLu Scer\GAL4^GMR.PFa Scer\GAL4^how-24B Scer\GAL4^Mef2.5xCD Scer\GAL4^Nep4.meso Scer\GAL4^VGlut-OK371
Constructs (17)
	P{Act5C-GAL4} P{GAL4-elav.L} P{GD5655} P{GD5710} P{GMR-GAL4.w^-} P{KK102673} P{KK104462} P{Mef2-GAL4.5xCD} P{Nep4.A-HA} P{Nep4-eGFP.meso} P{Nep4-GAL4.meso} P{UAS-Nep4.A.FExxH} P{UAS-Nep4.A.HExxF} P{UAS-Nep4.A.HQxxH} P{UAS-Nep4.A.trunc} P{UAS-Nep4.A} P{UAS-Nep4.B}
Genes (9)
	Avic\GFP Ca-P60A CG3534 dlg1 Nep1 Nep4 Scer\GAL4 T:Ivir\HA1 T:nls-tra
Insertions (3)
	P{EPgy2}Nep1^EY21255 P{GawB}how^24B P{GawB}VGlut^OK371
Natural transposons (1)
	P-element