Monica Miele scite author profile

IC50 for S247 adhesion to alpha(v)beta3 or alpha(IIB)beta3a substrates was 0.2 nM vs. 244 nM, respectively. Likewise, S247 was not toxic at doses up to 1000 microM. However, osteoclast cultures treated with S247 exhibited marked morphological changes and impaired formation of the actin sealing zone. When S247 was administered prior to tumor cells, there was a significant, dose-dependent reduction (25-50% of vehicle-only-treated mice; P = 0.002) in osseous metastasis. Mice receiving S247 after tumor cell inoculation also developed fewer bone metastases, but the difference was not statistically significant. These data suggest that, in the MDA-MB-435 model, the alpha(v)beta3 integrin plays an important role in early events (e.g., arrest of tumor cells) in bone metastasis. Furthermore, the data suggest that alpha(v)beta3 inhibitors may be useful in the treatment and/or prevention of breast cancer metastases in bone.

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In vitro loss of heterozygosity targets the PTEN/MMAC1 gene in melanoma

Robertson

Furnari

Miele

et al. 1998

Proc. Natl. Acad. Sci. U.S.A.

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Gross genetic lesions of chromosome 10 occur in 30-50% of sporadic human melanomas. To test the functional significance of this observation, we have developed an in vitro loss of heterozygosity approach in which a wild-type chromosome 10 was transferred into melanoma cells, where there was selection for its breakage and regional deletion to relieve its growth suppressive effects. The overlap of these events was at band 10q23, the site of the recently isolated PTEN͞MMAC1 tumor suppressor gene, suggesting it as a potential target. Although the gene was expressed in the parental cells, both of its chromosomal alleles contained truncating mutations. In vitro loss of heterozygosity resulted in loss of the chromosomally introduced wild-type PTEN͞ MMAC1, and ectopic expression of the gene caused cell growth suppression. Thus, this approach identified PTEN͞MMAC1 as a target in malignant melanoma and may provide an alternative means to localizing tumor suppressor genes.

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Monica Miele

KiSS-1, a Novel Human Malignant Melanoma Metastasis-Suppressor Gene

Sex Hormones Modulate Inflammatory Mediators Produced by Macrophages^a

A small molecule antagonist of the α_vβ₃integrin suppresses MDA-MB-435 skeletal metastasis

In vitro loss of heterozygosity targets the PTEN/MMAC1 gene in melanoma

Contact Info

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Resources

About

Monica Miele

KiSS-1, a Novel Human Malignant Melanoma Metastasis-Suppressor Gene

Sex Hormones Modulate Inflammatory Mediators Produced by Macrophagesa

A small molecule antagonist of the αvβ3integrin suppresses MDA-MB-435 skeletal metastasis

In vitro loss of heterozygosity targets the PTEN/MMAC1 gene in melanoma

Contact Info

Product

Resources

About

Sex Hormones Modulate Inflammatory Mediators Produced by Macrophages^a

A small molecule antagonist of the α_vβ₃integrin suppresses MDA-MB-435 skeletal metastasis