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PubMed:12972803 JSONTXT

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DisGeNET

Id Subject Object Predicate Lexical cue
T0 643-647 gene:1719 denotes DHFR
T1 721-724 disease:C0023448 denotes ALL
T2 643-647 gene:1719 denotes DHFR
T3 771-777 disease:C0006826 denotes Cancer
T4 643-647 gene:1719 denotes DHFR
T5 771-777 disease:C1306459 denotes Cancer
R1 T0 T1 associated_with DHFR,ALL
R2 T2 T3 associated_with DHFR,Cancer
R3 T4 T5 associated_with DHFR,Cancer

PubMed_Structured_Abstracts

Id Subject Object Predicate Lexical cue
T1 155-575 OBJECTIVE denotes Methotrexate is a major component of current treatment regimens for children with acute lymphocytic leukemia (ALL). Potential mechanisms of methotrexate resistance include impaired drug uptake, decreased drug retention, and dihydrofolate reductase (DHFR) amplification. The purpose of this study was to assess whether reduced folate carrier (RFC) and DHFR expression in untreated leukemic blasts correlated with outcome.
T2 585-792 METHODS denotes Quantitative real-time RT-PCR was used to measure RFC and DHFR mRNA expression in leukemic blasts from 40 newly diagnosed patients with ALL obtained in a blinded fashion from Children's Cancer Group studies.
T3 802-1247 RESULTS denotes Low RFC expression at diagnosis correlated significantly with an unfavorable event free survival. Surprisingly, low, not high, DHFR expression correlated significantly with an unfavorable event-free survival. Proliferative cell nuclear antigen (PCNA) expression demonstrated a weak inverse relationship between sample PCNA and DHFR or RFC expression, suggesting that DHFR and RFC expression may be markers for factors other than drug resistance.
T4 1261-1572 CONCLUSIONS denotes These results suggest that impaired transport may be an important mechanism of intrinsic methotrexate resistance in ALL, and DHFR expression also may be an important prognostic factor in ALL. Additional studies are necessary to clarify the mechanism for the correlation of low DHFR expression with poor outcome.