LOX-1 abrogation reduces cardiac hypertrophy and collagen accumulation following chronic ischemia in the mouse

Lu, Jianrong; Wang, X; Wang, W; Muniyappa, Harish; Hu, Chang Ping; Mitra, Sona; Long, Bo; Das, Kumuda C.; Mehta, J. L.

doi:10.1038/gt.2011.133

Cited by 49 publications

(39 citation statements)

References 35 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Besides chronic ischemia, LOX1 may also be detrimental for cardiac damage that occurs in ischemia-reperfusion. Specifi cally, LOX-1 increased in rat cardiomyocytes following ischemia-reperfusion, while administration of anti-LOX-1 antibody reduced myocardial infarction size [ 120 ] and LOX-1 genetic deletion reduced ischemia-driven collagen accumulation [ 121 ]. Therefore, LOX-1 appears to be involved in ischemic heart failure as it activates stress signaling kinases, such as JNK and ERK [ 112 ].…”

Section: Ischemiamentioning

confidence: 97%

See 1 more Smart Citation

Lipoproteins: A Source of Cardiac Lipids

Drosatos

Goldberg

2014

Cardiac Energy Metabolism in Health and Disease

View full text Add to dashboard Cite

Lipids are the major substrate for cardiac ATP production and they are derived from adipose tissue or lipoprotein triglycerides. Lipoproteins are synthesized in the liver and they obtain their mature form following interaction with enzymes that are present in the circulation. Lipoprotein-derived fatty acids are released by lipoprotein lipase and are then taken up by cardiomyocytes either passively or via fatty acid receptors, such as CD36. Uptake of remnant lipoproteins via cardiomyocyte lipoprotein receptors is also possible. Besides fatty acids, other hydrophobic molecules such as cholesteryl esters, retinyl esters and vitamins are delivered by lipoproteins to the heart. While lipids are important for normal cardiac function, excessive lipid uptake, also known as lipotoxicity, may lead to cardiac abnormalities. This chapter focuses on the role of lipoproteins in providing fatty acids and other essential lipids to the heart in healthy conditions as well as in cardiac disease.

show abstract

Section: Ischemiamentioning

confidence: 97%

“…Abrogation of LOX-1 in an animal model of chronic ischemia reduced infarct size, improved cardiac hemodynamics, prevented cardiac remodeling and fi brosis and improved survival [ 121 ]. Besides chronic ischemia, LOX1 may also be detrimental for cardiac damage that occurs in ischemia-reperfusion.…”

Section: Ischemiamentioning

confidence: 98%

Lipoproteins: A Source of Cardiac Lipids

Drosatos

Goldberg

2014

Cardiac Energy Metabolism in Health and Disease

View full text Add to dashboard Cite

show abstract

“…The homozygous LOX-1 KO mice were developed and backcrossed eight times with C57BL/6 strain to replace the genetic background [8,11]. This investigation conforms to the Guide for the Care and Use of Laboratory Animals published by the US National Institutes of Health (NIH Publication No.…”

Section: Animal Protocolmentioning

confidence: 99%

“…In recent studies, LOX-1 deletion was shown to limit cardiac hypertrophy and the remodeling process in mice subjected to sustained hypertension or myocardial ischemia. [8][9][10] Part of the decrease in cardiac remodeling with LOX-1 deletion seems to be related to reduction in fibrosis in the heart. 8 In view of markedly reduced collagen deposition and fibrosis in the LOX-1 knockout (KO) mice hearts, we posited that LOX-1 may modulate fibroblast growth, a key factor for cardiac fibrosis.…”

mentioning

confidence: 99%

Lectin-like Oxidized Low-density Lipoprotein Receptor-1 (LOX-1) and Cardiac Fibroblast Growth

et al. 2012

View full text Add to dashboard Cite

Abstract-Lectin-like oxidized low-density lipoprotein receptor-1 (LOX-1) regulates growth of a variety of cells and is important in inflammation, oxidative stress, and tissue remodeling. Recent studies show that LOX-1 deletion limits cardiac remodeling after sustained hypertension. We posited that LOX-1 may affect cardiac fibroblast growth and collagen secretion. To examine this postulate, we studied growth pattern of cardiac fibroblasts from hearts of wild-type and LOX-1 knockout (KO) mice. LOX-1 KO fibroblasts exhibited dramatically reduced growth when compared with wild-type mice fibroblasts and became much larger than wild-type mice fibroblasts in serial cultures, suggesting arrest of cell division. Western blotting and immunofluorescence showed that cell division control protein 42, a key regulator for cell division, was markedly downregulated in LOX-1 KO fibroblasts. The cytoskeletal organization in these fibroblasts was significantly altered in strand orientation, and some fibroblasts were completely devoid of F-actin. Furthermore, NADPH oxidase expression and generation of reactive oxygen species, as well as cell proliferation signals serine/threonine-specific protein kinase and murine double minute 2, were significantly reduced in LOX-1 KO fibroblasts. To confirm the essential role of LOX-1 in fibroblast growth, LOX-1 KO fibroblasts were transfected with h-LOX-1 cDNA. After transfection, the altered pattern of cytoskeletal organization, as well as expression of cell division control protein 42, serine/threonine-specific protein kinase, and murine double minute 2, was normalized. In congruent with these in vitro data, we found that the cardiac fibroblast number and expression of fibronectin and procoallagen-1/collagen were significantly lower in hypertensive LOX-1 KO mice hearts than in hypertensive wild-type mice hearts subjected to sustained hypertension (angiotensin II infusion).

show abstract

“…Кроме того, есть данные, что мЛПНП сами по себе могут вступать во взаимодей-ствие и активировать СРБ [19]. Важно отметить, что, кроме активации системы комплемента, LOX-1 [20] и СРБ [21] могут сами непосредственно участвовать в фиброзе миокарда. Таким образом, повышение уров-ня мЛПНП запускает многофакторные процессы, которые в конечном итоге могут приводить к фиброзу миокарда.…”

unclassified

Modified Low-Density Lipoprot Eins in Di Abetes Mellitus Type 2

Драпкина¹,

Gegenava²

2018

Klinicist

View full text Add to dashboard Cite

Objective:to compare the level of modified low-density lipoproteins (mLDL) in patients with diabetes mellitus type 2 (DM2) and without DM2; to identify the factors affecting mLDL сontent.Materials and methods.The study involved 64 patients; they were divided into 2 groups. The main group included 32 patients with DM2 (15 men and 17 women, median age – 65 years), the control group 2 included 32 patients without DM2 (15 men and 17 women, median age – 60.5 years). All patients (100 %) had arterial hypertension. Both groups were generally comparable in the main clinical and laboratory characteristics. Mann–Whitney test, Spearman correlation coefficient were used for statistical data processing.Results. In patients with DM2 mLDL level was significantly higher (р <0.001) and correlated with blood glucose concentration (p = 0.021), glycated hemoglobin values (p <0.001) and body-weight index (p = 0.007). In patients without DM2 mLDL level correlated with bodyweight index (p <0.001). No correlation between mLDL level and standard LDL content was found in patients with DM2 and in patients without DM2 (p = 0.714 and p = 0.758 respectively).Conclusion.DM2 is significantly associated with an increased mLDL level that is affected by parameters of carbohydrate metabolism and body-weight index. In persons without hyperlipidemia mLDL level increases in case of hyperglycemia.

show abstract

LOX-1 abrogation reduces cardiac hypertrophy and collagen accumulation following chronic ischemia in the mouse

Cited by 49 publications

References 35 publications

Lipoproteins: A Source of Cardiac Lipids

Lipoproteins: A Source of Cardiac Lipids

Lectin-like Oxidized Low-density Lipoprotein Receptor-1 (LOX-1) and Cardiac Fibroblast Growth

Modified Low-Density Lipoprot Eins in Di Abetes Mellitus Type 2

Contact Info

Product

Resources

About