Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
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Target Concepts:
Gene/Protein
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Query: UMLS:C0278883 (
metastatic melanoma
)
6,224
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Coculture of human melanocytes with keratinocytes upregulates
CCN3
, a matricellular protein critical to maintenance of normal homeostasis of melanocytes in the skin.
CCN3
affects two fundamental features of melanocyte physiology: it inhibits melanocyte proliferation and stimulates their adhesion to the basement membrane. Here we report that expression of
CCN3
is downregulated in advanced melanomas. Aggressive melanoma cell lines did not respond to treatment with
CCN3
inducers, such as interleukin-1beta (IL-1beta), while less aggressive melanoma cell lines responded similarly to melanocytes. Immunostaining analyses revealed that
CCN3
was present in melanoma cells close to the epidermal-dermal interface, but not in melanoma cells that had invaded deep into the dermis or had metastasized to lymph nodes. Contrary to our expectations, overexpression of
CCN3
in 1205Lu
metastatic melanoma
cells did not affect their adhesion to collagen IV. However,
CCN3
decreased the transcription and activation of matrix metalloproteinases and suppressed the invasion of 1205Lu melanoma cells. These results suggest that the lack of
CCN3
in advanced melanoma cells contributes to their invasive phenotype. Whereas major matricellular proteins, such as osteopontin, tenascin or secreted protein acidic and rich in cysteine (SPARC), are strongly upregulated in melanoma cells;
CCN3
is the first member of this family that is downregulated.
...
PMID:Downregulation of CCN3 expression as a potential mechanism for melanoma progression. 1796 13
CCN3
/nephroblastoma overexpressed belongs to the CCN family of genes that encode secreted proteins associated with the extracellular matrix (ECM) and exert regulatory effects at the cellular level. Overexpression of
CCN3
was shown in
metastatic melanoma
cells compared with cells of the primary tumor from the same patient. Analysis of short-term cultures from 50 primary and metastatic melanomas revealed a heterogeneous expression pattern of both the 46-kDa full-length cytoplasmic/secreted protein and the 32-kDa nuclear-truncated form. The different protein expression patterns were not associated with gene alterations or polymorphisms. Like the metastatic cells expressing high levels of the 46-kDa
CCN3
, cells transfected to overexpress
CCN3
showed increased adhesion to ECM proteins, whereas inhibition of
CCN3
expression by small interfering RNA decreased adhesion to laminin and vitronectin.
CCN3
overexpression induced increased expression of laminin and vitronectin integrin receptors alpha 7 beta 1 and alpha v beta 5 by increasing their mRNA production. Moreover,
CCN3
secreted by melanoma cells acted as an adhesion matrix protein for melanoma cells themselves. Analysis of
CCN3
protein expression with respect to melanoma progression detected the protein in all visceral metastases tested and in most nodal metastases from relapsing patients but in only a few nodal metastases from nonrelapsing patients and cutaneous metastases. Consistently, xenotransplantation in immunodeficient mice showed a higher metastatic potential of melanoma cells overexpressing
CCN3
. Together, these data indicate a role for
CCN3
in melanoma cell interaction with the ECM by regulating integrin expression, resulting in altered cell adhesion and leading melanoma progression to aggressive disease.
...
PMID:CCN3/nephroblastoma overexpressed matricellular protein regulates integrin expression, adhesion, and dissemination in melanoma. 1824 71
