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Overexpression
of c-kit oncogene in human brain tumors
Landonio Giuseppe, Riva Maurizio, Galli Carlo, Schiavo
Roberta, Carminati Ornella, Secondino Simona, Gambacorta Marcello, Defanti Carlo
Alberto, Siena Salvatore
Depts of Oncology, Neurology, and Pathology-Ospedale
Niguarda Ca Granda, Milano, Italy.
Background
and Objective. In a systematic search for potential targets of new
molecular cancer therapies, we evaluated c-kit expression in human primary brain
tumors.
c-kit, a 145-kd transmembrane glycoprotein, has a close structural homology with
the kinase domains of platelet-derived growth factor receptor (PDGFr),
implicated in the pathogenesis of various primary brain tumors.
An activation of tyrosine kinase receptor and the association with some
identical second messenger system for c-kit activity and PDGFr were
demonstrated. Experimental findings show that STI-571 selectively inhibits c-kit
activity and downstream activation of target proteins, involved in cellular
proliferation.
Methods.
We evaluated c-kit expression by immunocytochemistry in paraffin embedded tumors
of 15 adults with high-grade glioma (2 PNET patients, 13 supratentorial
glioblastoma).
Well-differentiated oligodendroglioma or astrocytoma component was also
associated to high-grade glioma in 5/15.
WHO classification, histologic grading, and MIB-1 growth fraction were also
evaluated.
Results.
Intense, weak, and absent expression of c-kit was found 8 (2 PNET, 6
glioblastoma), 5 (4 glioblastoma mixed with well differentiated glioma),and 2 (1
glioblastoma, 1 glioblastoma mixed with grade II oligodendroglioma) cases,
respectively.
The pattern of c-kit positivity was perivascular around normal and new
microvessels for glioblastoma and diffuse for PNET.
Tumor growth fraction ranged from 10% to 60% (median 40%) among intense-positivity
cases and from 5 to 50% (median 25%) among weak-positivity cases.
Conclusions.
Correlation between the presence of c-kit expression and a more aggressive
malignancy was present in our cases; a predominant perivascular distribution was
also present in patients with glioblastoma.
Present data further motivate the therapeutic evaluation of c-kit targeted
therapies for brain high grade gliomas.
© Copyright 2002
American Society of Clinical Oncology
Source:
http://www.asco.org/ac/1,1003,_12-002324-00_18-002002-00_19-00295-00_29-00A-00_42-00ONeill-00_43-00-00_44-00-00_45-00
Author-00_46-00Title-00_47-00Title-00_48-00and-00_49-00and,00.asp?cat=CNS+Tumors&parent=CENTRAL+NERVOUS+SYSTEM+TUMORS
&returnpid=2323
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