Polymorphisms in the ABCB1 gene and effect on outcome and toxicity in childhood acute lymphoblastic leukemia

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作者
J Gregers
H Gréen
I J Christensen
K Dalhoff
H Schroeder
N Carlsen
S Rosthoej
B Lausen
K Schmiegelow
C Peterson
机构
[1] Clinical Pharmacology,Division of Drug Research, Department of Medical and Health Sciences
[2] Faculty of Health Sciences,Department of Clinical Immunology 7631
[3] Linköpings Universitet,Division of Gene Technology
[4] Laboratory of Molecular Medicine,Department of Forensic Genetics and Forensic Toxicology
[5] Rigshospitalet,Department of Clinical Pharmacology
[6] University Hospital in Copenhagen,Department of Pediatric
[7] Science for Life Laboratory,Department of Pediatric
[8] School of Biotechnology,Department of Pediatric
[9] KTH Royal Institute of Technology,Department of Pediatrics and Adolescent Medicine
[10] National Board of Forensic Medicine,undefined
[11] The Finsen Laboratory,undefined
[12] Rigshospitalet,undefined
[13] Bispebjerg Hospital,undefined
[14] University Hospital in Skejby,undefined
[15] University Hospital in Odense,undefined
[16] University Hospital in Aalborg,undefined
[17] Rigshospitalet,undefined
[18] University of Copenhagen,undefined
[19] Copenhagen,undefined
[20] Denmark,undefined
[21] The Medical Faculty,undefined
[22] Institute of Gynecology,undefined
[23] Obstetrics and Pediatrics,undefined
[24] University of Copenhagen,undefined
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摘要
The membrane transporter P-glycoprotein, encoded by the ABCB1 gene, influences the pharmacokinetics of anti-cancer drugs. We hypothesized that variants of ABCB1 affect outcome and toxicity in childhood acute lymphoblastic leukemia (ALL). We studied 522 Danish children with ALL, 93% of all those eligible. Risk of relapse was increased 2.9-fold for patients with the 1199GA variant versus 1199GG (P=0.001), and reduced 61% and 40%, respectively, for patients with the 3435CT or 3435TT variants versus 3435CC (overall P=0.02). The degree of bone marrow toxicity during doxorubicin, vincristine and prednisolone induction therapy was more prominent in patients with 3435TT variant versus 3435CT/3435CC (P=0.01/P<0.0001). We observed more liver toxicity after high-dose methotrexate in patients with 3435CC variant versus 3435CT/TT (P=0.03). In conclusion, there is a statistically significant association between ABCB1 polymorphisms, efficacy and toxicity in the treatment of ALL, and ABCB1 1199G>A may be a new possible predictive marker for outcome in childhood ALL.
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页码:372 / 379
页数:7
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