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Biochemical correlates of temozolomide sensitivity in pediatric solid tumor xenograft models.

Publication ,  Journal Article
Middlemas, DS; Stewart, CF; Kirstein, MN; Poquette, C; Friedman, HS; Houghton, PJ; Brent, TP
Published in: Clin Cancer Res
March 2000

The antitumor activity of the methylating agent temozolomide has been evaluated against a panel of 17 xenografts derived from pediatric solid tumors. Temozolomide was administered p.o. daily for five consecutive days at a dose level of 66 mg/kg. Courses of treatment were repeated every 21 days for three cycles. Tumor lines were classified as having high, intermediate, or low sensitivity, determined by complete responses, partial responses, or stable disease, respectively. Overall, temozolomide induced complete responses in five lines and partial responses in three additional tumor lines, giving objective regressions in 47% of xenograft lines. Analysis of temozolomide plasma systemic exposure indicated that this dose level was relevant to exposure achieved in patients. Tumors were analyzed by immunoblotting for levels of O6-methylguanine-DNA methyltransferase (MGMT) and two mismatch repair proteins, MLH-1 and MSH-2. Tumors classified as having high or intermediate sensitivity had low or undetectable MGMT and expressed detectable MLH-1 and MSH-2 proteins. Tumors classified as having low sensitivity had either (a) high MGMT or (b) low or undetectable MGMT but were deficient in MLH-1. The relationship between p53 and response to temozolomide was also examined. In vitro temozolomide did not induce p21cip1 in p53-competent NB-1643 neuroblastoma cells. Suppression of p53 function in NB1643 clones through stable expression of a trans dominant negative p53 (NB1643p53TDN) did not confer temozolomide resistance. Similarly, tumor sensitivity to temozolomide did not segregate with p53 genotype or p53 functional status. These results indicate that MGMT is the primary mechanism for temozolomide resistance, but in the absence of MGMT, proficient mismatch repair determines sensitivity to this agent.

Duke Scholars

Published In

Clin Cancer Res

ISSN

1078-0432

Publication Date

March 2000

Volume

6

Issue

3

Start / End Page

998 / 1007

Location

United States

Related Subject Headings

  • Tumor Suppressor Protein p53
  • Tumor Cells, Cultured
  • Transplantation, Heterologous
  • Temozolomide
  • Rhabdomyosarcoma
  • Proto-Oncogene Proteins
  • Phenotype
  • Oncology & Carcinogenesis
  • O(6)-Methylguanine-DNA Methyltransferase
  • Nuclear Proteins
 

Citation

APA
Chicago
ICMJE
MLA
NLM
Middlemas, D. S., Stewart, C. F., Kirstein, M. N., Poquette, C., Friedman, H. S., Houghton, P. J., & Brent, T. P. (2000). Biochemical correlates of temozolomide sensitivity in pediatric solid tumor xenograft models. Clin Cancer Res, 6(3), 998–1007.
Middlemas, D. S., C. F. Stewart, M. N. Kirstein, C. Poquette, H. S. Friedman, P. J. Houghton, and T. P. Brent. “Biochemical correlates of temozolomide sensitivity in pediatric solid tumor xenograft models.Clin Cancer Res 6, no. 3 (March 2000): 998–1007.
Middlemas DS, Stewart CF, Kirstein MN, Poquette C, Friedman HS, Houghton PJ, et al. Biochemical correlates of temozolomide sensitivity in pediatric solid tumor xenograft models. Clin Cancer Res. 2000 Mar;6(3):998–1007.
Middlemas, D. S., et al. “Biochemical correlates of temozolomide sensitivity in pediatric solid tumor xenograft models.Clin Cancer Res, vol. 6, no. 3, Mar. 2000, pp. 998–1007.
Middlemas DS, Stewart CF, Kirstein MN, Poquette C, Friedman HS, Houghton PJ, Brent TP. Biochemical correlates of temozolomide sensitivity in pediatric solid tumor xenograft models. Clin Cancer Res. 2000 Mar;6(3):998–1007.

Published In

Clin Cancer Res

ISSN

1078-0432

Publication Date

March 2000

Volume

6

Issue

3

Start / End Page

998 / 1007

Location

United States

Related Subject Headings

  • Tumor Suppressor Protein p53
  • Tumor Cells, Cultured
  • Transplantation, Heterologous
  • Temozolomide
  • Rhabdomyosarcoma
  • Proto-Oncogene Proteins
  • Phenotype
  • Oncology & Carcinogenesis
  • O(6)-Methylguanine-DNA Methyltransferase
  • Nuclear Proteins