Study of the Individual Cytochrome b5 and Cytochrome b5 Reductase Domains of Ncb5or Reveals a Unique Heme Pocket and a Possible Role of the CS Domain

Deng, Bin; Parthasarathy, Sudharsan; Wang, Wenfang; Gibney, Brian R.; Battaile, Kevin P.; Lovell, Scott; Benson, David R.; Zhu, Hao

doi:10.1074/jbc.m110.120329

Cited by 34 publications

(38 citation statements)

References 69 publications

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“…Hepatocytes of Ncb5or knockout mice have an increased sensitivity to SFA-induced damage, which can be at least partly attributed to a lower SCD-specific activity in these cells [27] . This observation strongly supports the hypothesized functional link between SCD1 and Ncb5or [8] . Some natural human mutations of NCB5OR have been reported to remarkably decrease the level of active enzyme due to enhanced proteasomal degradation [28] ; therefore, the potential role of this gene in human pathology deserves further investigation.…”

supporting

confidence: 88%

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Lipotoxicity in the liver

Zámbó

Simon-Szabó

Szelényi

et al. 2013

WJH

160

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Obesity due to excessive food intake and the lack of physical activity is becoming one of the most serious public health problems of the 21 st century. With the increasing prevalence of obesity, non-alcoholic fatty liver disease is also emerging as a pandemic. While previously this pathophysiological condition was mainly attributed to triglyceride accumulation in hepatocytes, recent data show that the development of oxidative stress, lipid peroxidation, cell death, inflammation and fibrosis are mostly due to accumulation of fatty acids, and the altered composition of membrane phospholipids. In fact, triglyceride accumulation might play a protective role, and the higher toxicity of saturated or trans fatty acids seems to be the consequence of a blockade in triglyceride synthesis. Increased membrane saturation can profoundly disturb cellular homeostasis by impairing the function of membrane receptors, channels and transporters. However, it also induces endoplasmic reticulum stress via novel sensing mechanisms of the organelle's stress receptors. The triggered signaling pathways in turn largely contribute to the development of insulin resistance and apoptosis. These findings have substantiated the lipotoxic liver injury hypothesis for the pathomechanism of hepatosteatosis. This minireview focuses on the metabolic and redox aspects of lipotoxicity and lipoapoptosis, with special regards on the involvement of endoplasmic reticulum stress responses. Key words: Saturated fatty acid; Lipotoxicity; Steatosis; Lipoapoptosis; Endoplasmic reticulum stress Core tip: Surplus of free fatty acids contributes to hepatic injuries in obesity and type 2 diabetes. Intracellular accumulation of fatty acyl-CoA causes oxidative and endoplasmic reticulum (ER) stress, which lead to cell death, inflammation and fibrosis. Steatohepatosis is the consequence of an intensive fat synthesis, aiming to reduce the metabolic burden. The higher toxicity of saturated vs unsaturated fatty acids is partly due to a limited capacity of the liver cells to insert them into triglycerides. Moreover, increased membrane saturation triggers the ER stress response though a unique mechanism, which aggravates the metabolic derangements and liver injuries.

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supporting

confidence: 88%

“…to participate in fatty acid desaturation [8] . Membrane lipid saturation is regulated through the activity of various lysophospolipid acyltransferase enzymes exhibiting different acyl-CoA specificities.…”

Section: Fatty Acid Metabolism In the Livermentioning

confidence: 99%

Lipotoxicity in the liver

Zámbó

Simon-Szabó

Szelényi

et al. 2013

WJH

160

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“…Ncb5or readily reduces a variety of artificial substrates in vitro in the presence of excess NADH or NADPH, as does the Cyb5A⅐Cyb5R3 complex (1,11,12). Ncb5or is a more potent electron donor than Cyb5A because of the lower redox potential (E 0 ϭ Ϫ108 mV) in the Ncb5or heme center (11) and its unique heme environment (13). Of four recognized missense mutations in the human Ncb5or gene, two (Q187R and H223R) are found in a cohort with non-autoimmune diabetes (14).…”

mentioning

confidence: 99%

Ncb5or Deficiency Increases Fatty Acid Catabolism and Oxidative Stress

Xu¹,

Wang

Frontera³

et al. 2011

Journal of Biological Chemistry

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“…In this complex, it became clear that shortening the CPR hinge region leads to a protein that favors the open conformation and promotes association with HO (Sugishima et al, 2014). These studies demonstrate the utility of combining the power of Sevrioukova et al, 1997Cupp-Vickery et al, 2000;Hall et al, 2001;Podust et al, 2001;Yoshinari et al, 2001;Williams et al, 2003;Grahn et al, 2006;He et al, 2006;Deng et al, 2010;Wilderman et al, 2012;Hiruma et al, 2013;Tripathi et al, 2013;Peng et al, 2014;Sugishima et al, 2014;Basudhar et al, 2015;Reed and Backes, 2017;Gill, 1983;Kakuta et al, 1997;Meech and Mackenzie, 1997;Argiriadi et al, 1999;Binda et al, 2001Binda et al, , 2011…”

Section: X-ray Crystallographymentioning

confidence: 83%

“…In an X-ray crystallography study comparing the b 5 -like protein, Ncb5or, with b 5 , Deng et al determined that the positioning of the second histidine heme ligand (His 112) in b 5 is critical for efficient electron transfer, both from b 5 reductase and to the (CYP) electron transfer partner (Figure 1; Deng et al, 2010). These are just a few of the many examples available where X-ray crystallography has been used to interrogate CYP and electron transfer partner interactions.…”

Section: Measurement Of Intermolecular Binding Constants and Reactionmentioning

confidence: 99%