Bridging the molecular and biological functions of the oxysterol-binding protein family

Pietrangelo, Antonietta; Ridgway, Neale D.

doi:10.1007/s00018-018-2795-y

Cited by 78 publications

(93 citation statements)

References 159 publications

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“…In 2010, Shair et al reported that OSBP and ORP4 L, two members of the oxysterol binding protein (ORP) superfamily implicated in lipid/sterol transport and sensing are the major protein targets of OSW-1. [4,5] Using competitive binding assays based on recombinant OSBP and ORP4 L and [ 3 H]-25-HC, their endogenous ligand, OSW-1 exhibits high affinity toward these proteins (K i = 26 nM for OSBP and 54 nM for ORP4 L). However, the link between the inhibition of OSBP and ORP4 L and apoptotic induction has remained unclear.…”

Section: Introductionmentioning

confidence: 99%

Development of Chemical Probes for Functional Analysis of Anticancer Saponin OSW‐1

Komatsu

Sakurai

2019

The Chemical Record

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Chemical probe‐based approaches have proven powerful in recent years in the target identification studies of natural products. OSW‐1 is a saponin class of natural products with highly potent and selective cytotoxicity against various cancer cell lines. Understanding its mechanism of action is important for the development of anticancer drugs with potentially novel target pathways. This account reviews recent progress in the development of OSW‐1 derived probes for exploring the mechanism of its action. The key to the probe development is a judicious choice of functionalization sites and a selective functionalization strategy. The types of probes include fluorescent probes for cellular imaging analysis and affinity probes for target identification analysis.

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Section: Introductionmentioning

confidence: 99%

Development of Chemical Probes for Functional Analysis of Anticancer Saponin OSW‐1

Komatsu

Sakurai

2019

The Chemical Record

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“…Therefore, the long-term, compound-induced reduction of OSBP in cells presents a new route to broad spectrum anti-Enterovirus activity, including as a novel route to antiviral prophylactic treatment through small molecule targeting a human host protein.O xysterol-binding protein (OSBP) and the OSBP-related proteins (ORPs) are a family of lipid and sterol binding proteins conserved in all eukaryotes. 1,2 The 12 OSBP/ORP human proteins share a conserved ∼50 kDa, C-terminal ligand binding domain. 1,2 OSBP and ORP4, the member most closely related to OSBP, share substantial sequence similarity, and both contain N-terminal pleckstrin homology (PH) and FFAT domains.…”

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confidence: 99%

“…3−5 The PH and FFAT domains alter OSBP cellular localization upon binding of ligands in the C-terminal ligand binding domain. 1,2 OSBP binding partners, including several regulatory proteins, have been reported. 1,2 OSBP gene expression and protein regulation are not well-defined.…”

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confidence: 99%

“…2,10 OSBP is expressed in all tissues, but ORP4 is expressed in only a few select human tissues. 1,2 ORP4 is highly expressed in some cancer cells and shown to be required for cancer cell line proliferation. 2,10 ORP4 is selectively overex- Figure 1.…”

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confidence: 99%

“…1,2 ORP4 is highly expressed in some cancer cells and shown to be required for cancer cell line proliferation. 2,10 ORP4 is selectively overex- Figure 1. Brief exposure to nontoxic, low-nanomolar OSW-1 compound concentrations causes long-term OSBP reduction in multiple cell lines.…”

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confidence: 99%

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Transient Compound Treatment Induces a Multigenerational Reduction of Oxysterol-Binding Protein (OSBP) Levels and Prophylactic Antiviral Activity

et al. 2018

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Oxysterol-binding protein (OSBP) is a lipid transport and regulatory protein required for the replication of Enterovirus genus viruses, which includes many significant human pathogens. Short-term exposure (i.e., 1−6 h) to a low dose (i.e., 1 nM) of the natural product compound OSW-1 induces a reduction of cellular OSBP levels by ∼90% in multiple different cell lines with no measurable cytotoxicity, defect in cellular proliferation, or global proteome reduction. Interestingly, the reduction of OSBP levels persists multiple days after the low-dose, transient OSW-1 compound treatment is ended and the intracellular OSW-1 compound levels drop to undetectable levels. The reduction in OSBP levels is inherited in multiple generations of cells that are propagated after the OSW-1 compound treatment is stopped. The enduring multiday, multigenerational reduction of OSBP levels triggered by the OSW-1 compound is not due to proteasome degradation of OSBP or due to a reduction in OSBP mRNA levels. OSW-1 compound treatment induces transient autophagy in cells, but blocking autophagy does not rescue OSBP levels. Although the specific cellular mechanism of long-term OSBP repression is not yet identified, these results clearly show the existence of an OSBP specific cellular regulation process that is triggered upon treatment with an OSBP-binding compound. The stable reduction of OSBP levels upon short-term, transient OSW-1 compound treatment will be a powerful tool to understand OSBP regulation and cellular function. Additionally, the persistent reduction in OSBP levels triggered by the transient OSW-1 compound treatment substantially reduces viral replication in treated cells. Therefore, the long-term, compound-induced reduction of OSBP in cells presents a new route to broad spectrum anti-Enterovirus activity, including as a novel route to antiviral prophylactic treatment through small molecule targeting a human host protein.O xysterol-binding protein (OSBP) and the OSBP-related proteins (ORPs) are a family of lipid and sterol binding proteins conserved in all eukaryotes. 1,2 The 12 OSBP/ORP human proteins share a conserved ∼50 kDa, C-terminal ligand binding domain. 1,2 OSBP and ORP4, the member most closely related to OSBP, share substantial sequence similarity, and both contain N-terminal pleckstrin homology (PH) and FFAT domains. 1,2 Individual OSBP/ORP family members are reported to have many different cellular functions, 1,2 including serving as cellular sensors for lipid membrane composition. 3−6 OSBP is reported to be localized at the membrane contact site between the ER and Golgi, and from this location, OSBP is

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May we target double‐membrane vesicles and oxysterol‐binding protein to combat SARS‐CoV‐2 infection?

Shahmohamadnejad

Nabavi

Habtemariam

et al. 2020

Cell Biology International

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Bridging the molecular and biological functions of the oxysterol-binding protein family

Cited by 78 publications

References 159 publications

Development of Chemical Probes for Functional Analysis of Anticancer Saponin OSW‐1

Development of Chemical Probes for Functional Analysis of Anticancer Saponin OSW‐1

Transient Compound Treatment Induces a Multigenerational Reduction of Oxysterol-Binding Protein (OSBP) Levels and Prophylactic Antiviral Activity

May we target double‐membrane vesicles and oxysterol‐binding protein to combat SARS‐CoV‐2 infection?

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