Margot P. Cleary scite author profile

There is now substantial evidence that overweight and/or obesity and/or weight gain are risk factors for the development of postmenopausal breast cancer. In addition, obesity and/or elevated body mass index at breast cancer diagnosis has a negative impact on prognosis for both premenopausal and postmenopausal women. Therefore, understanding the mechanism of how obesity affects the mammary tumorigenesis process is an important health issue. Elevated serum estrogen levels as well as enhanced local production of estrogen have been considered primary mediators of how increased body weight promotes breast cancer development in postmenopausal women. Here, we provide an overview of estrogen's relationship with both obesity and breast cancer as separate entities. Human and relevant preclinical studies are cited. In addition, other growth factors that may be involved in this relationship are considered.

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Treatment of hyperlipidemia reduces glomerular injury in obese Zucker rats

Kasiske

O’Donnell

Cleary

et al. 1988

Kidney International

415

179

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Hyperlipidemic obese Zucker rats develop albuminuria and spontaneous focal glomerulosclerosis (FGS) at an early age, despite normal glomerular capillary pressures and nephron plasma flows. To investigate the role of abnormal lipid metabolism in the pathogenesis of FGS, pharmacologic agents were used to reduce serum lipids in male, obese Zucker rats. Eight rats were treated from 8 to 40 weeks of age with the cholesterol synthesis inhibitor, mevinolin (group I). A separate group of seven obese rats was treated with the structurally-unrelated lipid lowering agent, clofibric acid (group II). Results from these two groups were compared to controls injected with vehicle only (group III). Body weight and food intake were similar in all three groups. Mevinolin reduced both serum cholesterol and fasting triglyceride levels while clofibric acid lowered only serum cholesterol. Urine albumin excretion was reduced in groups I and II compared to group III. Mesangial matrix expansion and cellularity were both reduced by mevinolin and clofibric acid. In addition, the percent of glomeruli with focal glomerulosclerosis was much less in groups I (0.4 +/- 0.1%) and II (1.3 +/- 0.7%) compared to group III (4.6 +/- 0.7%, P less than 0.05). Micropuncture studies, carried out in separate groups of obese rats, demonstrated that mevinolin and clofibric acid did not affect glomerular hemodynamic function. Although the precise mechanism remains to be defined, these results suggest that abnormal lipid metabolism may be important in the pathogenesis of FGS.

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Margot P. Cleary

Leptin--A Growth Factor in Normal and Malignant Breast Cells and for Normal Mammary Gland Development

Obesity and Breast Cancer: The Estrogen Connection

Treatment of hyperlipidemia reduces glomerular injury in obese Zucker rats

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