Cargo binding promotes KDEL receptor clustering at the mammalian cell surface

Becker, Björn; Shaebani, M. Reza; Rammo, Domenik; Bubel, Tobias; Santen, Ludger

doi:10.1038/srep28940

Cited by 30 publications

(38 citation statements)

References 42 publications

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“…2 c). These results demonstrate that Hsp47 uptake by cells is dependent on KDEL receptor display on the cell membrane, as suggested in earlier reports [46].…”

Section: Resultssupporting

confidence: 91%

“…Hsp47 is retained in the ER via KDEL receptor mediated transport from the Golgi to the ER [26,30,[41][42][43][44][45]. This KDEL-receptor is also found on the cell membrane, [46] and is critical for the uptake of exogenous Hsp47 and transport to the ER of cells by simply adding the protein to the culture medium [23]. Expression levels of KDEL receptor at the cell membrane are cell-dependent [47,48].…”

Section: Introductionmentioning

confidence: 99%

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Exogenous supply of Hsp47 triggers fibrillar collagen deposition in skin cell cultures in vitro

Khan

Sankaran

Llontop

et al. 2020

BMC Mol and Cell Biol

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Background: Collagen is a structural protein that provides mechanical stability and defined architectures to skin. In collagen-based skin disorders this stability is lost, either due to mutations in collagens or in the chaperones involved in collagen assembly. This leads to chronic wounds, skin fragility, and blistering. Existing approaches to treat such conditions rely on administration of small molecules to simulate collagen production, like 4phenylbutyrate (4-PBA) or growth factors like TGF-β. However, these molecules are not specific for collagen synthesis, and result in unsolicited side effects. Hsp47 is a collagen-specific chaperone with a major role in collagen biosynthesis. Expression levels of Hsp47 correlate with collagen deposition. This article explores the stimulation of collagen deposition by exogenously supplied Hsp47 (collagen specific chaperone) to skin cells, including specific collagen subtypes quantification. Results: Here we quantify the collagen deposition level and the types of deposited collagens after Hsp47 stimulation in different in vitro cultures of cells from human skin tissue (fibroblasts NHDF, keratinocytes HaCat and endothelial cells HDMEC) and mouse fibroblasts (L929 and MEF). We find upregulated deposition of fibrillar collagen subtypes I, III and V after Hsp47 delivery. Network collagen IV deposition was enhanced in HaCat and HDMECs, while fibril-associated collagen XII was not affected by the increased intracellular Hsp47 levels. The deposition levels of fibrillar collagen were cell-dependent i.e. Hsp47-stimulated fibroblasts deposited significantly higher amount of fibrillar collagen than Hsp47-stimulated HaCat and HDMECs. Conclusions: A 3-fold enhancement of collagen deposition was observed in fibroblasts upon repeated dosage of Hsp47 within the first 6 days of culture. Our results provide fundamental understanding towards the idea of using Hsp47 as therapeutic protein to treat collagen disorders.

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“…2 c). These results demonstrate that Hsp47 uptake by cells is dependent on KDEL receptor display on the cell membrane, as suggested in earlier reports [46].…”

Section: Resultssupporting

confidence: 91%

Section: Introductionmentioning

confidence: 99%

Exogenous supply of Hsp47 triggers fibrillar collagen deposition in skin cell cultures in vitro

Khan

Sankaran

Llontop

et al. 2020

BMC Mol and Cell Biol

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“…Consistent with these results, CTB-KDEL and CTB have shown comparable GM1binding affinity in ELISA, surface plasmon resonance, and flow cytometry analysis using the mouse macrophage cell line RAW264.7 [89]. Together, these results indicate that CTB-KDEL, but not CTB, facilitates TGFβ-mediated epithelial wound healing in the [108][109][110], it was hypothesized that CTB-KDEL could localize and remain in the ER for an extended period after retrograde transport [54]. To test this hypothesis, Caco2 cells were treated with CTB-KDEL or CTB then washed and incubated for 0, 12, 24 hours, followed by an immunoblot analysis to detect CTB and CTB-KDEL in the cell lysates.…”

Section: The C-terminal Kdel Sequence Is Essential For the Colon Epitsupporting

confidence: 75%

A recombinant cholera toxin b subunit variant (CTB-KDEL) exhibits unique colon mucosal healing effects that have therapeutic implications for inflammatory bowel disease.

Royal¹

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“…This motif is recognized by KDEL receptor after Hsp47 release in the Golgi and is responsible for its retention in the ER 41 KDEL sequence has been shown to block the retention of Hsp47 into the ER 42 . The KDEL receptor is also present in the plasma membrane of cells, and has been shown to assist internalization of KDEL containing molecules from the extracellular space [43][44][45] . We tested if our Hsp47 variants could be delivered to ER using KDEL receptormediated endocytosis (Fig.3).…”

Section: Hsp47 Variants Can Be Delivered Into Er Via Kdel Receptor-mementioning

confidence: 99%

Photoactivatable Hsp47: A Tool to Control and Regulate Collagen Secretion & Assembly

Khan¹,

Sankaran²,

Paez³

et al. 2018

Preprint

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Hsp47 is a chaperone protein with a fundamental role in the folding, stability and intracellular transport of procollagen triple helices. A light-responsive Hsp47 recombinant protein, engineered to control in situ the production and assembly of cellular collagen is here demonstrated. This novel light-driven tool enables unprecedented fundamental studies of collagen biosynthesis and associated diseases.

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Cargo binding promotes KDEL receptor clustering at the mammalian cell surface

Cited by 30 publications

References 42 publications

Exogenous supply of Hsp47 triggers fibrillar collagen deposition in skin cell cultures in vitro

Exogenous supply of Hsp47 triggers fibrillar collagen deposition in skin cell cultures in vitro

A recombinant cholera toxin b subunit variant (CTB-KDEL) exhibits unique colon mucosal healing effects that have therapeutic implications for inflammatory bowel disease.

Photoactivatable Hsp47: A Tool to Control and Regulate Collagen Secretion & Assembly

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