Absence of Caveolin-1 Sensitizes Mouse Skin to Carcinogen-Induced Epidermal Hyperplasia and Tumor Formation

Capozza, Franco; Williams, Terence M.; Schubert, William; McClain, Steve A.; Bouzahzah, Boumediene; Sotgia, Federica; Lisanti, Michael P.

doi:10.1016/s0002-9440(10)64335-0

Cited by 152 publications

(134 citation statements)

References 44 publications

(40 reference statements)

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“…Also, Caveolin-1 expression is reduced in several human tumors, including lung [29], mammary [30], colon [15,31] and ovarian carcinomas [32], as well as sarcomas [32] and re-expression of Caveolin-1 often (but not always) results in reversal of characteristics associated with the transformed phenotype. Consistent with these results, lung hyperplasia and predisposition to mammary, as well as carcinogen-induced skin hyperplasia and tumor formation are observed in Caveolin-1 knock-out mice [4][5][33][34][35]. These results indicate that Caveolin-1 displays properties and characteristics of a tumor suppressor molecule in a variety of cellular settings.…”

Section: The Tumor Suppressor Hypothesissupporting

confidence: 73%

“…In NIH3T3 fibroblasts, down-regulation of Caveolin-1 using specific siRNA is sufficient to hyperactivate the MAPK/ERK pathway and induce cell transformation [78]. Also, in Caveolin-1 knock-out mice, signaling via the MAPK/ERK pathway is increased and associated with increased sensitivity to topically applied carcinogens, cardiac hypertrophy and neointimal hyperplasia [33,[87][88]. Moreover, in human head and neck squamous cell cancer, Caveolin-1 inhibits the ERK pathway and cell growth [89], and in human laryngeal carcinoma cell lines, Caveolin-1 interaction with the EGFR is associated with reduced MAPK/ERK phosphorylation and increased apoptotic cell death [90].…”

Section: The Ras/raf/erk Connectionmentioning

confidence: 99%

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The Caveolin-1 Connection to Cell Death and Survival

Quest

Lobos-González²,

Núñez³

et al. 2013

Current Molecular Medicine

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Abstract:Caveolins are a family of membrane proteins required for the formation of small plasma membrane invaginations called caveolae that are implicated in cellular trafficking processes. In addition to this structural role, these scaffolding proteins modulate numerous intracellular signaling pathways; often via direct interaction with specific binding partners. Caveolin-1 is particularly well-studied in this respect and has been attributed a large variety of functions. Thus, Caveolin-1 also represents the best-characterized isoform of this family with respect to its participation in cancer. Rather strikingly, available evidence indicates that Caveolin-1 belongs to a select group of proteins that function, depending on the cellular settings, both as tumor suppressor and promoter of cellular traits commonly associated with enhanced malignant behavior, such as metastasis and multi-drug resistance. The mechanisms underlying such ambiguity in Caveolin-1 function constitute an area of great interest. Here, we will focus on discussing how Caveolin-1 modulates cell death and survival pathways and how this may contribute to a better understanding of the ambiguous role this protein plays in cancer.

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Section: The Tumor Suppressor Hypothesissupporting

confidence: 73%

Section: The Ras/raf/erk Connectionmentioning

confidence: 99%

The Caveolin-1 Connection to Cell Death and Survival

Quest

Lobos-González²,

Núñez³

et al. 2013

Current Molecular Medicine

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“…However, caveolin-1 has also been found to be downregulated in tumours themselves, and several independent studies have shown that the re-expression of caveolin-1 in transformed cells inhibits features of the transformed phenotype, such as anchorage-independent growth. Caveolin-1 knockout mice also support the hypothesis, as they display hyperproliferative disorders and hyperactivation of the MAPK cascade, and are at greater risk from carcinogeninduced tumorigenesis [188]. Although these mice do not spontaneously form tumours, knockouts of important cell cycle control agents, such as the cyclin-dependent kinase inhibitor p21, also do not form tumours [206].…”

Section: Caveolin-1 Levels Are Not Always Reduced In Transformed Cellsmentioning

confidence: 79%

“…In addition, Capozza et al [188] found that caveolin-1 knockout mice were more susceptible to skin carcinogenesis induced by a known carcinogen, 7,12-dimethylbenzanthracene (DMBA).…”

Section: Caveolin Knockout Micementioning

confidence: 99%

Lipid Rafts and Caveolae in Signaling by Growth Factor Receptors

Laurentiis¹,

Donovan²,

Arcaro³

2007

TOBIOCJ

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Lipid rafts and caveolae are microdomains of the plasma membrane enriched in sphingolipids and cholesterol, and hence are less fluid than the remainder of the membrane. Caveolae have an invaginated structure, while lipid rafts are flat regions of the membrane. The two types of microdomains have different protein compositions (growth factor receptors and their downstream molecules) suggesting that lipid rafts and caveolae have a role in the regulation of signaling by these receptors. The purpose of this review is to discuss this model, and the implications that it might have regarding a potential role for lipid rafts and caveolae in human cancer. Particular attention will be paid to the epidermal growth factor receptor, for which the largest amount of information is available. It has been proposed that caveolins act as tumor suppressors. The role of lipid rafts is less clear, but they seem to be capable of acting as 'signaling platforms', in which signal initiation and propagation can occur efficiently.

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“…54 In addition, Cav-1-deficient mice show the same phenotype, with increased ketone body production systemically 48 and increased numbers of stem cells in the skin, gut, mammary gland and brain. [55][56][57][58][59][60] In the brain, astrocytes produce mitochondrial fuels (L-lactate, ketone bodies and glutamine), which are then consumed by oxidative mitochondrial metabolism in neurons. 61 In addition, Figure 13.…”

Section: Methodsmentioning

confidence: 99%