Critical Roles of Hydrophobicity and Orientation of Side Chains for Inactivation of Sarcoplasmic Reticulum Ca2+-ATPase with Thapsigargin and Thapsigargin Analogs

Winther, Anne-Marie Lund; Liu, Huizhen; Sonntag, Yonathan; Olesen, Claus; Maire, Marc le; Soehoel, Helmer; Olsen, Carl Erik; Christensen, Søren Brøgger; Nissen, Poul; Møller, Jesper

doi:10.1074/jbc.m110.136242

Cited by 86 publications

(107 citation statements)

References 48 publications

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“…X-ray structures of SERCA, corresponding to the E2 and the E2P forms, respectively, were used as starting structures for the protein. For the E2 conformation, a structure for a similar crystal form with a nortrilobolide inhibitor, refined at a higher resolution, was applied (PDB 3NAL 41 ). This structure has a Cα-RMSD of 0.5 Å to the E2 crystal structure reported here.…”

Section: Methodsmentioning

confidence: 99%

Mutual adaptation of a membrane protein and its lipid bilayer during conformational changes

et al. 2011

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The structural elucidation of membrane proteins continues to gather pace, but we know little about their molecular interactions with the lipid environment or how they interact with the surrounding bilayer. Here, with the aid of low-resolution X-ray crystallography, we present direct structural information on membrane interfaces as delineated by lipid phosphate groups surrounding the sarco(endo)plasmic reticulum Ca 2 + -ATPase (sERCA) in its phosphorylated and dephosphorylated Ca 2 + -free forms. The protein-lipid interactions are further analysed using molecular dynamics simulations. We find that sERCA adapts to membranes of different hydrophobic thicknesses by inducing local deformations in the lipid bilayers and by undergoing small rearrangements of the amino-acid side chains and helix tilts. These mutually adaptive interactions allow smooth transitions through large conformational changes associated with the transport cycle of sERCA, a strategy that may be of general nature for many membrane proteins.

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Section: Methodsmentioning

confidence: 99%

Mutual adaptation of a membrane protein and its lipid bilayer during conformational changes

et al. 2011

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“…A similar mechanism has been derived from structural data of Ca-ATPase. In E 2 , the headgroup of a PE molecule was identified between TM2, -4, -6, and -9 (58,59). In E 1 , this space is occupied by TM2, and the phospholipid is bound more superficially between TM2 and -9 (60).…”

mentioning

confidence: 99%

Stimulation, Inhibition, or Stabilization of Na,K-ATPase Caused by Specific Lipid Interactions at Distinct Sites

Habeck¹,

Haviv²,

Katz³

et al. 2015

Journal of Biological Chemistry

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Background: Na,K-ATPase is stabilized by phosphatidylserine/cholesterol and is stimulated by neutral phospholipids. Results: Three specific lipid-Na,K-ATPase interactions are detectable that either (a) stabilize the protein or (b) stimulate or (c) inhibit Na,K-ATPase activity, with distinct kinetic mechanisms. Conclusion: There are separate binding sites for phosphatidylserine/cholesterol (stabilizing), polyunsaturated phosphatidylethanolamine (stimulatory), and sphingomyelin/cholesterol (inhibitory). Significance: In physiological conditions, specifically bound lipids may regulate Na,K-ATPase activity.

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“…Thapsigargin (TG) is a natural product isolated from the seeds of Thapsia garganica L, which binds tightly to and inhibits the function of the transmembrane portion of the sarcoplasmic/endoplasmic reticulum calcium adenosine triphosphatase pump, inducing apoptosis (1,2). TG initiates endoplasmic reticulum (ER) stress via the unfolded protein response (UPR), which is initiated by 3 ER transmembrane proteins termed protein kinase-like endoplasmic reticulum kinase (PERK), inositol-requiring enzyme 1 (IRE1) and activating transcription factor (ATF) 6 (3,4).…”

Section: Introductionmentioning

confidence: 99%

HBV suppresses thapsigargin-induced apoptosis via inhibiting CHOP expression in hepatocellular carcinoma cells

Zhao

Liu

Liu³

et al. 2017

Oncology Letters

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Abstract. Hepatocellular carcinoma (HCC) accounts for a proportion of cancer-associated mortalities worldwide. Hepatitis B virus (HBV) infection is a major cause of HCC in China. Thapsigargin (TG) is a potential antitumor prodrug, eliciting endoplasmic reticulum (ER) stress via the inhibition of the ER calcium pump, effectively inducing apoptosis. The present study therefore examined the role of HBV in TG-induced apoptosis using two HCC cell lines, HBV positive HepG2.2.15 and HBV negative HepG2. When these two cell lines were treated with TG, HepG2.2.15 was less susceptible to apoptosis than HepG2. This phenomenon was confirmed by an MTT assay and Annexin V-FITC/propidium iodide staining. Reverse transcription quantitative polymerase chain reaction and western blotting were used to detect the expression levels of genes in the ER stress pathway subsequent to treatment with TG. Notably, the mRNA and protein levels of the apoptosis factor DNA damage inducible transcript 3 (CHOP) increased significantly in the HepG2 cells compared with the HepG2.2.15 cells. Additionally, the HepG2.2.15 cells treated with interferon-α exhibited higher levels of CHOP compared with the untreated cells. The overexpression or knockdown of CHOP microRNA in HepG2.2.15 or HepG2 cells may reduce the difference in apoptosis status between the two cell lines. These results suggest that HBV may inhibit the apoptosis induced by ER stress. These findings may be useful in the development of selective therapies for patients with HBV-positive tumors.

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Critical Roles of Hydrophobicity and Orientation of Side Chains for Inactivation of Sarcoplasmic Reticulum Ca2+-ATPase with Thapsigargin and Thapsigargin Analogs

Cited by 86 publications

References 48 publications

Mutual adaptation of a membrane protein and its lipid bilayer during conformational changes

Mutual adaptation of a membrane protein and its lipid bilayer during conformational changes

Stimulation, Inhibition, or Stabilization of Na,K-ATPase Caused by Specific Lipid Interactions at Distinct Sites

HBV suppresses thapsigargin-induced apoptosis via inhibiting CHOP expression in hepatocellular carcinoma cells

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