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Literature DB >> 32213546

Chronic Ethanol Feeding in Mice Decreases Expression of Genes for Major Structural Bone Proteins in a Nox4-Independent Manner.

Kim B Pedersen¹, Michelle L Osborn¹, Alex C Robertson¹, Ashlee E Williams¹, James Watt¹, Alexandra Denys¹, Katrin Schröder¹, Martin J Ronis².

Abstract

Bone loss in response to alcohol intake has previously been hypothesized to be mediated by excessive production of reactive oxygen species via NADPH oxidase (Nox) enzymes. Nox4 is one of several Nox enzymes expressed in bone. We investigated the role of Nox4 in the chondro-osteoblastic lineage of the long bones in mice during normal chow feeding and during chronic ethanol feeding for 90 days. We generated mice with a genotype (PrxCre +/- Nox4 fl/fl) allowing conditional knockout of Nox4 in the limb bud mesenchyme. Adult mice had 95% knockdown of Nox4 expression in the femoral shafts. For mice on regular chow, only whole-body Nox4 knockout mice had clearly increased cortical thickness and bone mineral density in the tibiae. When chronically fed a liquid diet with and without ethanol, conditional Nox4 knockout mice had slightly reduced dimensions of the cortical and trabecular regions of the tibiae (P < 0.1). The ethanol diet caused a significant reduction in cortical bone area and cortical thickness relative to a control diet without ethanol (P < 0.05). The ethanol diet further reduced gene expression of Frizzled related protein (Frzb), myosin heavy chain 3, and several genes encoding collagen and other major structural bone proteins (P < 0.05), whereas the Nox4 genotype had no effects on these genes. In conclusion, Nox4 expression from both mesenchymal and nonmesenchymal cell lineages appears to exert subtle effects on bone. However, chronic ethanol feeding reduces cortical bone mass and cortical gene expression of major structural bone proteins in a Nox4-independent manner. SIGNIFICANCE STATEMENT: Excessive alcohol intake contributes to osteopenia and osteoporosis, with oxidative stress caused by the activity of NADPH oxidases hypothesized to be a mediator. We tested the role of NADPH oxidase (Nox) 4 in osteoblast precursors in the long bones of mice with a conditional Nox4 knockout model. We found that Nox4 exerted effects independent of alcohol intake, and ethanol effects on bone were Nox4-independent.

Entities: Chemical Disease Gene Species

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Year: 2020 PMID： 32213546 PMCID： PMC7228502 DOI： 10.1124/jpet.119.264374

Source DB: PubMed Journal: J Pharmacol Exp Ther ISSN： 0022-3565 Impact factor: 4.030

15 in total

1. Inhibition of NADPH oxidases prevents chronic ethanol-induced bone loss in female rats.

Authors: Jin-Ran Chen; Oxana P Lazarenko; Kartik Shankar; Michael L Blackburn; Charles K Lumpkin; Thomas M Badger; Martin J J Ronis
Journal: J Pharmacol Exp Ther Date: 2010-11-22 Impact factor: 4.030

2. Knockout of the Gsta4 Gene in Male Mice Leads to an Altered Pattern of Hepatic Protein Carbonylation and Enhanced Inflammation Following Chronic Consumption of an Ethanol Diet.

Authors: Colin T Shearn; Casey F Pulliam; Kim Pedersen; Kyle Meredith; Kelly E Mercer; Laura M Saba; David J Orlicky; Martin J Ronis; Dennis R Petersen
Journal: Alcohol Clin Exp Res Date: 2018-05-30 Impact factor: 3.455

3. NOX4 Deletion in Male Mice Exacerbates the Effect of Ethanol on Trabecular Bone and Osteoblastogenesis.

Authors: James Watt; Alexander W Alund; Casey F Pulliam; Kelly E Mercer; Larry J Suva; Jin-Ran Chen; Martin J J Ronis
Journal: J Pharmacol Exp Ther Date: 2018-04-13 Impact factor: 4.030

4. Reduced Serum Osteocalcin in High-Risk Alcohol Using People Living With HIV Does Not Correlate With Systemic Oxidative Stress or Inflammation: Data From the New Orleans Alcohol Use in HIV Study.

Authors: James Watt; Jonathan Schuon; Jacob Davis; Tekeda F Ferguson; David A Welsh; Patricia E Molina; Martin J J Ronis
Journal: Alcohol Clin Exp Res Date: 2019-10-01 Impact factor: 3.455

5. Partial Protection by Dietary Antioxidants Against Ethanol-Induced Osteopenia and Changes in Bone Morphology in Female Mice.

Authors: Alexander W Alund; Kelly E Mercer; Casey F Pulliam; Larry J Suva; Jin-Ran Chen; Thomas M Badger; Martin J J Ronis
Journal: Alcohol Clin Exp Res Date: 2016-12-17 Impact factor: 3.455

6. NADPH oxidase 4 limits bone mass by promoting osteoclastogenesis.

Authors: Claudia Goettsch; Andrea Babelova; Olivia Trummer; Reinhold G Erben; Martina Rauner; Stefan Rammelt; Norbert Weissmann; Valeska Weinberger; Sebastian Benkhoff; Marian Kampschulte; Barbara Obermayer-Pietsch; Lorenz C Hofbauer; Ralf P Brandes; Katrin Schröder
Journal: J Clin Invest Date: 2013-11 Impact factor: 14.808

Review 7. Cellular and molecular mechanisms of alcohol-induced osteopenia.

Authors: Zhenhua Luo; Yao Liu; Yitong Liu; Hui Chen; Songtao Shi; Yi Liu
Journal: Cell Mol Life Sci Date: 2017-07-03 Impact factor: 9.261

8. Protein-altering MYH3 variants are associated with a spectrum of phenotypes extending to spondylocarpotarsal synostosis syndrome.

Authors: Raphael Carapito; Alice Goldenberg; Nicodème Paul; Angélique Pichot; Albert David; Antoine Hamel; Clémentine Dumant-Forest; Julien Leroux; Benjamin Ory; Bertrand Isidor; Seiamak Bahram
Journal: Eur J Hum Genet Date: 2016-07-06 Impact factor: 4.246

9. Loss of functional NADPH oxidase 2 protects against alcohol-induced bone resorption in female p47phox-/- mice.

Authors: Kelly E Mercer; Clark R Sims; Carrie S Yang; Rebecca A Wynne; Christopher Moutos; William R Hogue; Charles K Lumpkin; Larry J Suva; Jin-Ran Chen; Thomas M Badger; Martin J J Ronis
Journal: Alcohol Clin Exp Res Date: 2013-11-20 Impact factor: 3.455

10. The Gene Ontology Resource: 20 years and still GOing strong.

Authors:
Journal: Nucleic Acids Res Date: 2019-01-08 Impact factor: 16.971

5 in total

1. Binge Ethanol Exposure in Mice Represses Expression of Genes Involved in Osteoblast Function and Induces Expression of Genes Involved in Osteoclast Differentiation Independently of Endogenous Catalase.

Authors: Alexandra Denys; Kim B Pedersen; James Watt; Allison R Norman; Michelle L Osborn; Jin-Ran Chen; Cole Maimone; Shana Littleton; Vasilis Vasiliou; Martin J J Ronis
Journal: Toxicol Sci Date: 2022-01-24 Impact factor: 4.109

5. Declining serum bone turnover markers are associated with the short-term positive change of lumbar spine bone mineral density in postmenopausal women.

Authors: Shengli Zhao; Xiaoyi Mo; Zhenxing Wen; Ming Liu; Zhipeng Chen; Wei Lin; Zifang Huang; Bailing Chen
Journal: Menopause Date: 2022-01-31 Impact factor: 3.310