Author
Listed:
- Bo Dong
(Laboratory for Morphogenetic Signaling, Riken Center for Developmental Biology)
- Ken Kakihara
(Laboratory for Morphogenetic Signaling, Riken Center for Developmental Biology
Kobe University Graduate School of Science
Present address: CTC Laboratory Systems Corporation, 16-7, 1-chome Komazawa, Setagaya-ku, Tokyo, 154-0012, Japan)
- Tetsuhisa Otani
(Laboratory for Morphogenetic Signaling, Riken Center for Developmental Biology)
- Housei Wada
(Laboratory for Morphogenetic Signaling, Riken Center for Developmental Biology)
- Shigeo Hayashi
(Laboratory for Morphogenetic Signaling, Riken Center for Developmental Biology
Kobe University Graduate School of Science)
Abstract
Apical extracellular matrix filling the lumen controls the morphology and geometry of epithelial tubes during development, yet the regulation of luminal protein composition and its role in tube morphogenesis are not well understood. Here we show that an endosomal-retrieval machinery consisting of Rab9, retromer and actin nucleator WASH (Wiskott–Aldrich Syndrome Protein and SCAR Homolog) regulates selective recycling of the luminal protein Serpentine in the Drosophila trachea. Secreted Serpentine is endocytosed and sorted into the late endosome. Vps35, WASH and actin filaments differentially localize at the Rab9-enriched subdomains of the endosomal membrane, where Serpentine containing vesicles bud off. In Rab9, Vps35 and WASH mutants, Serpentine was secreted normally into the tracheal lumen, but the luminal quantities were depleted at later stages, resulting in excessively elongated tubes. In contrast, secretion of many luminal proteins was unaffected, suggesting that retrograde trafficking of a specific class of luminal proteins is a pivotal rate-limiting mechanism for continuous tube length regulation.
Suggested Citation
Bo Dong & Ken Kakihara & Tetsuhisa Otani & Housei Wada & Shigeo Hayashi, 2013.
"Rab9 and retromer regulate retrograde trafficking of luminal protein required for epithelial tube length control,"
Nature Communications, Nature, vol. 4(1), pages 1-12, June.
Handle:
RePEc:nat:natcom:v:4:y:2013:i:1:d:10.1038_ncomms2347
DOI: 10.1038/ncomms2347
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