Identification of cells initiating human melanomas

Schatton, Tobias; Murphy, Gëorge F.; Frank, Natasha Y.; Yamaura, Kazuo; Waaga-Gasser, Ana Maria; Gasser, Martin; Zhan, Qimin; Jordan, Stefan; Duncan, Lyn M.; Weishaupt, Carsten; Fuhlbrigge, Robert C.; Kupper, Thomas S.; Sayegh, Mohamed H.; Frank, Markus H.

doi:10.1038/nature06489

Cited by 1,284 publications

(1,357 citation statements)

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“…[5][6][7][8][9] As shown in Figure 1b, all cell lines generated tumorospheres, and flow cytometry analyses showed that CD44 þ CD24 À population was highly enriched in tumorospheres (Supplementary Figure S1A). We sorted CD44 þ CD24 À cells from spheres of prostate and breast cancer using fluorescence-activated cell sorting (FACS) and achieved a purity of 495% as judged by postsorting flow analysis (Figure 1c).…”

Section: Resultsmentioning

confidence: 91%

“…Collectively, our data suggest that both CSCs and spheres exhibited diverse stem cell-associated characteristics, consistent with previous reports. [5][6][7][8][9] CSCs overexpressed BAD with elevated phosphorylation. As CSCs are resistant to drugs 11 and phosphorylated BAD correlates with drug resistance in cancer patients, 25 we determined the level of BAD expression and phosphorylation in CSCs and tumorospheres.…”

Section: Resultsmentioning

confidence: 99%

“…1,2 Subsequently, CSCs have been identified in several cancers. [3][4][5][6][7][8][9][10] Accumulating evidence suggests that current cancer therapies can only shrink tumors as they target and kill the differentiated cancer (DC) cells, but are unable to target the rare CSC population. 11,12 Thus, despite a wealth of information on DC cells, the active survival and self-renewal pathways in CSCs have not been characterized thoroughly.…”

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confidence: 99%

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Targeting proapoptotic protein BAD inhibits survival and self-renewal of cancer stem cells

Sastry

Al-Muftah

et al. 2014

Cell Death Differ

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Emerging evidence suggests that the resistance of cancer stem cells (CSC) to many conventional therapies is one of the major limiting factors of cancer therapy efficacy. Identification of mechanisms responsible for survival and self-renewal of CSC will help design new therapeutic strategies that target and eliminate both differentiated cancer cells and CSC. Here we demonstrated the potential role of proapoptotic protein BAD in the biology of CSC in melanoma, prostate and breast cancers. We enriched CD44 þ /CD24 À cells (CSC) by tumorosphere formation and purified this population by FACS. Both spheres and CSC exhibited increased potential for proliferation, migration, invasion, sphere formation, anchorage-independent growth, as well as upregulation of several stem cell-associated markers. We showed that the phosphorylation of BAD is essential for the survival of CSC. Conversely, ectopic expression of a phosphorylation-deficient mutant BAD induced apoptosis in CSC. This effect was enhanced by treatment with a BH3-mimetic, ABT-737. Both pharmacological agents that inhibit survival kinases and growth factors that are involved in drug resistance delivered their respective cytotoxic and protective effects by modulating the BAD phosphorylation in CSC. Furthermore, the frequency and self-renewal capacity of CSC was significantly reduced by knocking down the BAD expression. Consistent with our in vitro results, significant phosphorylation of BAD was found in CD44 þ CSC of 83% breast tumor specimens. In addition, we also identified a positive correlation between BAD expression and disease stage in prostate cancer, suggesting a role of BAD in tumor advancement. Our studies unveil the role of BAD in the survival and self-renewal of CSC and propose BAD not only as an attractive target for cancer therapy but also as a marker of tumor progression.

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Section: Resultsmentioning

confidence: 91%

Section: Resultsmentioning

confidence: 99%

mentioning

confidence: 99%

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Targeting proapoptotic protein BAD inhibits survival and self-renewal of cancer stem cells

Sastry

Al-Muftah

et al. 2014

Cell Death Differ

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“…To this end, stem cell research has opened up new and intriguing horizons that may enable better understanding of development of cancer in general and melanoma in particular. [6][7][8][9] Stem cells are slowly proliferating self-renewing cells that are able to differentiate into cell types of multiple lineages (ie, multipotent stem cells) or of one lineage (ie, unipotent stem cells). Researchers have identified stem cells of melanocytic lineage in the human hair follicle, the epidermis, and recently also in the dermis.…”

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confidence: 99%

Three Roots of Melanoma

Zalaudek

Marghoob²,

Scope³

et al. 2008

Arch Dermatol

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EGURA ET AL 1 DESCRIBE MORPHOLOGIC FEAtures of melanomas with a nodular component using in vivo reflectance-mode confocal microscopy (RCM) and correlate these RCM findings with histopathologic findings. The most striking observation made by the investigators is the remarkable difference in epidermal involvement between nodular melanoma (NM) and superficial spreading melanoma (SSM) with a nodular component. At RCM, SSMs frequently showed epidermal disarrangement and pagetoid infiltration, whereas NMs exhibited a preserved epidermal pattern and few paget-

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“…When acute myeloid leukemia patients are re-examined after chemotherapy, the persistence of CD34 þ CD38 À cells (proposed to be LICs) predicts a high risk of relapse (van Rhenen et al, 2005). Similarly, the presence of stemness markers within the tumor cells of melanoma and breast cancer patients (ABCB5 þ and CD44 þ , respectively) correlates with a higher rate of cancer progression and poor prognosis (Shipitsin et al, 2007;Schatton et al, 2008). As highlighted above, the eradication of LICs in APL upon treatment with retinoic acid and arsenic supports the concept that agents targeting TICs will lead to complete cure.…”

Section: Novel Paradigms For Cancer Therapy V Pavet Et Almentioning

confidence: 99%

Towards novel paradigms for cancer therapy

et al. 2010

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Cancer is a complex progressive multistep disorder that results from the accumulation of genetic and epigenetic abnormalities, which lead to the transformation of normal cells into malignant derivatives. Despite enormous progress in the understanding of cancer biology including the decryption of multiple regulatory networks governing cell growth and death, and despite the possibility of analyzing (epi)genetic deregulation at the genome-wide scale, cancertargeted therapy is still the exception. In fact, to date there are still far too few examples of therapies leading to cure; treatment-derived toxicity is a major issue, and cancer remains to be one of the largest causes of death worldwide. The purpose of this review is to discuss the state of the art of cancer therapy with respect to the key issue of any treatment, namely its target selectivity. Therefore, we recapitulate and discuss current concepts and therapies targeting tumorspecific features, including oncofusion proteins, aberrant kinase activities and epigenetic tumor makeup. We analyze strategies designed to induce tumor-selective death such as the use of oncolytic virus, tumoricidal proteins (NS1, Eorf4, apoptin, HAMLET (human a-lactalbumin made lethal to tumor cells)) and activation of signaling pathways involved in tumor surveillance. We emphasize the potential of the tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) pathway, an essential component of the evolutionary developed defense systems that eradicate malignant cells. Finally, we discuss the necessity of targeting tumor-initiating cells (TICs) to avoid relapse and increase the chances of complete remission, and describe emerging concepts that might provide novel avenues for cancer therapy.

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Identification of cells initiating human melanomas

Cited by 1,284 publications

References 29 publications

Targeting proapoptotic protein BAD inhibits survival and self-renewal of cancer stem cells

Targeting proapoptotic protein BAD inhibits survival and self-renewal of cancer stem cells

Three Roots of Melanoma

Towards novel paradigms for cancer therapy

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