850458C

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Sphingomyelins Prevent Propagation of Lipid Peroxidation-LC-MS/MS Evaluation of Inhibition Mechanisms.

Giulia Coliva et al.

Molecules (Basel, Switzerland), 25(8) (2020-04-25)

Free radical driven lipid peroxidation is a chain reaction which can lead to oxidative degradation of biological membranes. Propagation vs. termination rates of peroxidation in biological membranes are determined by a variety of factors including fatty acyl chain composition, presence

Plant-derived phosphocholine facilitates cellular uptake of anti-pulmonary fibrotic HJT-sRNA-m7.

Jianchao Du et al.

Science China. Life sciences, 62(3), 309-320 (2017-04-06)

Pulmonary fibrosis, a progressive chronic disease with a high mortality rate, has limited treatment options. Currently, lung transplantation remains the only effective treatment. Here we report that a small RNA, HJT-sRNA-m7, from a Chinese herbal medicine Hong Jing Tian (HJT

Cell-free synthesis and functional characterization of sphingolipid synthases from parasitic trypanosomatid protozoa.

Elitza S Sevova et al.

The Journal of biological chemistry, 285(27), 20580-20587 (2010-05-12)

The Trypanosoma brucei genome has four highly similar genes encoding sphingolipid synthases (TbSLS1-4). TbSLSs are polytopic membrane proteins that are essential for viability of the pathogenic bloodstream stage of this human protozoan parasite and, consequently, can be considered as potential

Lubricating recovery of damaged pleural mesothelium: effect of time and of phosphatidylcholines.

Francesca Bodega et al.

Respiratory physiology & neurobiology, 203, 116-120 (2014-08-17)

Effect of time and phosphatidylcholines (PCs) on lubrication of damaged mesothelium has been investigated. Marked increase in coefficient of kinetic friction (μ) of pleural specimens after mesothelial blotting and rewetting decreased by 23.4±3.5%, 41.8±3.8%, and 40.5±2.7% after 30min, 1h, and

Drugs Repurposed as Antiferroptosis Agents Suppress Organ Damage, Including AKI, by Functioning as Lipid Peroxyl Radical Scavengers.

Eikan Mishima et al.

Journal of the American Society of Nephrology : JASN, 31(2), 280-296 (2019-11-27)

Ferroptosis, nonapoptotic cell death mediated by free radical reactions and driven by the oxidative degradation of lipids, is a therapeutic target because of its role in organ damage, including AKI. Ferroptosis-causing radicals that are targeted by ferroptosis suppressors have not

Selective covalent targeting of GPX4 using masked nitrile-oxide electrophiles.

John K Eaton et al.

Nature chemical biology, 16(5), 497-506 (2020-04-02)

We recently described glutathione peroxidase 4 (GPX4) as a promising target for killing therapy-resistant cancer cells via ferroptosis. The onset of therapy resistance by multiple types of treatment results in a stable cell state marked by high levels of polyunsaturated

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