Statins Are Associated With Reduced Mortality in Multiple Myeloma

Sanfilippo, Kristen M.; Keller, Jesse; Gage, Brian F.; Luo, Suhong; Wang, Tzu‐Fei; Moskowitz, Gerald; Gumbel, Jason H.; Blue, Brandon; O’Brian, Katiuscia; Carson, Kenneth R.

doi:10.1200/jco.2016.68.3482

Cited by 79 publications

(64 citation statements)

References 36 publications

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“…Thus, the mevalonate pathway promotes tumorigenesis by two mechanisms: (1) by enhancing protein prenylation, which is required for the activation of proteins involved in proliferation and migration, such as Ras and Rho; and (2) by stabilizing conformational mutant p53. It should be noted that the efficacy of statins (cholesterol lowering drugs) that inhibit the mevalonate pathway on tumor suppression is promising, yet they still remain controversial [68,69,70,71,72]. Our study may suggest the importance of knowledge of the p53 status in tumors treated with statins to determine their efficacy.…”

Section: Summary and Future Perspectivesmentioning

confidence: 78%

p53 as a Regulator of Lipid Metabolism in Cancer

Parrales

Iwakuma

2016

IJMS

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Enhanced proliferation and survival are common features of cancer cells. Cancer cells are metabolically reprogrammed which aids in their survival in nutrient-poor environments. Indeed, changes in metabolism of glucose and glutamine are essential for tumor progression. Thus, metabolic reprogramming is now well accepted as a hallmark of cancer. Recent findings suggest that reprogramming of lipid metabolism also occurs in cancer cells, since lipids are used for biosynthesis of membranes, post-translational modifications, second messengers for signal transduction, and as a source of energy during nutrient deprivation. The tumor suppressor p53 is a transcription factor that controls the expression of proteins involved in cell cycle arrest, DNA repair, apoptosis, and senescence. p53 also regulates cellular metabolism, which appears to play a key role in its tumor suppressive activities. In this review article, we summarize non-canonical functions of wild-type and mutant p53 on lipid metabolism and discuss their association with cancer progression.

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Section: Summary and Future Perspectivesmentioning

confidence: 78%

p53 as a Regulator of Lipid Metabolism in Cancer

Parrales

Iwakuma

2016

IJMS

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“…Patients receiving statins for at least 5 years have been found to have a 47% lower risk of colorectal cancer than non-statin users, after adjustment for other known risk factors 97 . In another study, statins decreased patient mortality across various cancer types, regardless of whether they were taken before or after cancer diagnosis [98][99][100][101] . Experiments on leiomyoma have shown that simvastatin treatment not only inhibits cell proliferation and enhances cell apoptosis, but also suppresses levels of extracellular matrix proteins 102 .…”

Section: Targeting Cholesterol Metabolism For Cancer Therapymentioning

confidence: 96%

Cholesterol metabolism in cancer: mechanisms and therapeutic opportunities

2020

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C holesterol is vital for the survival and growth of mammalian cells. More than a membrane constituent, cholesterol is a precursor to bile acids and steroid hormones, which can initiate or promote colon, breast and prostate cancers 1-3 . Cholesterol can also modulate signalling pathways involved in tumourigenesis and cancer progression by covalently modifying proteins including hedgehog and smoothened 4,5 , and by facilitating the formation of specialized membrane microdomains 6,7 . Brief overview of cholesterol metabolismEvery mammalian cell can synthesize cholesterol through the mevalonate pathway (Fig. 1a). Two acetyl-CoA molecules in the cytosol condense, thus forming acetoacetyl-CoA, which reacts with the third acetyl-CoA and yields 3-hydroxy-3-methylglutaryl-CoA (HMG-CoA). HMG-CoA is reduced to mevalonate by HMG-CoA reductase (HMGCR), the primary rate-limiting enzyme in cholesterol biosynthesis. A series of enzymatic reactions convert mevalonate to farnesyl pyrophosphate (FPP), a precursor of sterols and all non-sterol isoprenoids. The condensation of two FPP molecules to squalene commits the process to sterol production. FPP also gives rise to geranylgeranyl pyrophosphate (GGPP), and both FPP and GGPP can prenylate and activate several oncogenic proteins such as Ras 8 . Squalene is then oxidized by squalene epoxidase (SQLE) to 2,3-epoxysqualene, which is cyclized to lanosterol. In the next steps, lanosterol follows the Bloch pathway, the Kandutsch-Russell pathway or a hybrid pathway before it is finally converted to cholesterol.Beyond de novo cholesterol biosynthesis, most cells acquire cholesterol from low-density lipoprotein (LDL) taken up from the circulation via LDL receptor (LDLR)-mediated endocytosis 9 . Enterocytes absorb dietary cholesterol from the intestinal lumen in a process involving the cholesterol transporter NPC1L1, the clathrin adaptor NUMB and the adaptor protein LIMA1 (refs. 10-12 ). Cholesterol within the cell is dynamically transported, reaching the destined membranes for structural and functional needs 13 . Cholesterol in excess of the current cellular demand is either exported from the cell by ATP-binding cassette (ABC) transporters, Reprogrammed cholesterol metabolism in cancer cellsHallmark features of cancer cholesterol metabolism. As fastproliferating cells, cancer cells require high levels of cholesterol for membrane biogenesis and other functional needs. For example, the cholesterol-derived oncometabolite 6-oxo-cholestan-3β,5α-diol, which is enriched in patients with breast cancer, binds glucocorticoid receptors and subsequently promotes tumour growth 19 . In general, cholesterol metabolism substantially contributes to cancer progression, including cell proliferation, migration and invasion 20-23 .Cholesterol metabolism produces essential membrane components as well as metabolites with a variety of biological functions. In the tumour microenvironment, cell-intrinsic and cell-extrinsic cues reprogram cholesterol metabolism and consequently promote tumourigenesis. Cholesterol-de...

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“…116,117 Recently, a large study of more than 4000 veterans with multiple myeloma demonstrated a 12-month overall survival advantage in individuals with multiple myeloma on a statin. 118 Similarly, in a large study by Nielsen and colleagues 119 of the Danish population with a cancer diagnosis between 1995 and 2007, there was a reduced cancer mortality among statin users compared with those who had never used statins in 13 different types of cancers (adjusted HR for death of any cause 0.82; 95% CI, 0.81–0.85).…”

Section: Cardiac Risk Factors and Cancer Outcomesmentioning

confidence: 97%

Cardio-oncology Related to Heart Failure

Blaes

Prizment

Koene

et al. 2017

Heart Failure Clinics

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Summary There are many similar risk factors for both cancer and cardiovascular disease. There are substantial biological data to support the hypotheses that the pathogenesis of these 2 diseases overlaps. Exercise should be strongly encouraged and should continue to be a focus of ongoing research. The management of risk factors for cardiovascular disease and cancer, including tobacco use, a healthy diet, and normal weight, should be further addressed. Treatment of cardiac risk factors, including hypertension, hyperlipidemia, and diabetes, in cancer patients may actually improve overall outcomes not only in cancer patients on active therapy but also in cancer survivors. As a result, continued collaboration between oncology and cardiology is essential.

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Statins Are Associated With Reduced Mortality in Multiple Myeloma

Cited by 79 publications

References 36 publications

p53 as a Regulator of Lipid Metabolism in Cancer

p53 as a Regulator of Lipid Metabolism in Cancer

Cholesterol metabolism in cancer: mechanisms and therapeutic opportunities

Cardio-oncology Related to Heart Failure

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