Methods for optimizing clinical responsiveness to methotrexate therapy using metabolite profiling and pharmacogenetics

a metabolite profiling and clinical responsiveness technology, applied in the field of medical genetics, can solve the problems of inability to use as cofactors, dna biosynthesis, cell division, etc., and achieve the effect of increasing the amount of chemotherapy

Inactive Publication Date: 2009-08-06
CYPRESS BIOSCI +1
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  • Summary
  • Abstract
  • Description
  • Claims
  • Application Information

AI Technical Summary

Problems solved by technology

Despite its structural similarity to folic acid, methotrexate cannot be used as a cofactor by enzymes that require folate, and instead competes with the folate cofactor for enzyme binding sites, thereby inhibiting protein and DNA biosynthesis and, hence, cell division.
Although methotrexate is among the best tolerated of the disease-modifying anti-rheumatic drugs (DMARDs), a major drawback of methotrexate therapy is a troublesome inter-patient variability in the clinical response and an unpredictable appearance of side effects including gastrointestinal disturbances, alopecia, elevation of liver enzymes, and bone marrow suppression (Weinblatt et al., Arthritis Rheum.
Thus, the lack of efficient therapeutic drug monitoring of methotrexate therapy and difficulty of rapidly individualizing methotrexate dose-maximizing response hampers effective patient treatment.
Moreover, a recent study of children with acute lymphoblastic leukemia has suggested that the A variant may be associated with poor clinical outcomes as compared with patients having the G / G genotype; individuals carrying the A / A genotype presented higher plasma concentrations of methotrexate compared to those with the G / G or G / A genotypes (Laverdiere et al., supra, 2002).

Method used

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  • Methods for optimizing clinical responsiveness to methotrexate therapy using metabolite profiling and pharmacogenetics
  • Methods for optimizing clinical responsiveness to methotrexate therapy using metabolite profiling and pharmacogenetics
  • Methods for optimizing clinical responsiveness to methotrexate therapy using metabolite profiling and pharmacogenetics

Examples

Experimental program
Comparison scheme
Effect test

example 1

Methotrexate Tri-Glutamate Concentrations can Predict Clinical Responsiveness to Chemotherapy

A. Methods

[0253]In this cross-sectional study, eligibility was limited to patients of at least 18 years of age who met the revised criteria of the American Rheumatism Association for Rheumatoid Arthritis and had received low dose methotrexate therapy for at least three months. Some patients were on additional medications for rheumatoid arthritis, including low dose corticosteroids (<10 mg day), and folic acid supplementation (1 mg / day). The Institutional Review Board approved the study, and patient consent was obtained.

[0254]Patient characteristics were collected at the time of the enrollment in the clinical study. Clinical assessment included a tender joint count, a swollen joint count, a Physician's Assessment of Disease Activity (using a 10 cm visual analog scale (VAS)), and a Patient's Assessment of Physical Function using the modified-Health Assessment Questionnaire (m-HAQ). The mHAQ is...

example 2

Genetic Polymorphisms Associated with Superior Clinical Responsiveness to Chemotherapy

[0262]This example describes the identification of novel associations between genetic polymorphisms in the folate, de novo purine synthesis, and de novo pyrimidine synthesis pathways and clinical responsiveness to chemotherapy.

A. Contribution of the RFC-1 G80A Polymorphism to Clinical Responsiveness to Methotrexate Therapy

[0263]In the 108 patients, allelic frequency for the RFC-1 80A variant allele was 44%. The distribution of genotypes consisted of 34 / 108 (31%) patients with the homozygous wild-type genotype (RFC-1 80G / G), 53 / 108 (49%) heterozygous patients (RFC-1 80G / A) and 21 / 108 (19%) patients with the homozygous mutant genotype (RFC-1 80A / A). The twenty-one patients carrying the RFC-1 homozygous mutant genotype (RFC-1 80A / A) were compared to the eighty-seven patients carrying the non-homozygous mutant genotype, which was either wild-type or heterozygous (RFC-1 80G / G or 80G / A).

[0264]As shown in...

example 3

An HPLC System Suitable for Detection of MTXPGs in Samples from Individuals Undergoing Methotrexate Therapy

[0277]This example describes a chromatographic system, conditions, and reagents suitable for separation of methotrexate polyglutamates (MTXPGs) in cell samples.

A. Preparation of Reagents

[0278]4-amino-10-methylpteroylglutamic acid (methotrexate; MTXPG1) was purchased from SIGMA (St. Louis, Mo.). 4-amino-10-methylpteroyldi-glutamic acid (MTXPG2), 4-amino-10-methylpteroyltri-glutamic acid (MTXPG3), 4-amino-10-methylpteroyltetra-glutamic acid (MTXPG4), 4-amino-10-methylpteroylpenta-glutamic acid (MTXPG5; SEQ ID NO:12), 4-amino-10-methylpteroylhexa-glutamic acid (MTXPG6; SEQ ID NO:15), and 4-amino-10-methylpteroylhepta-glutamic acid (MTXPG7; SEQ ID NO:14) were purchased as ammonium salts from Schircks laboratories (Jona, Switzerland). HPLC grade acetonitrile was purchased from Fisher Chemicals (Fair Lawn, N.J.); hydrogen peroxide (30%, v / v), ammonium hydroxide, and glacial acetic ac...

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Abstract

The present invention provides methods for optimizing clinical responsiveness to chemotherapy in an individual through genotypic analysis of polymorphisms in at least one gene. The methods of the present invention may further comprise determining the level of at least one long-chain methotrexate polyglutamate (MTXPG) in a sample obtained from the individual. The present invention also provides methods for generating a pharmacogenetic index for predicting clinical responsiveness to chemotherapy in an individual through genotypic analysis of polymorphisms in at least one gene. In addition, the present invention provides methods for optimizing therapeutic efficacy of chemotherapy in an individual by calculating the level of at least one long-chain MTXPG in a sample obtained from the individual.

Description

CROSS-REFERENCES TO RELATED APPLICATIONS[0001]This application is a Divisional App. and claims the benefit of the filing date of a U.S. Non-Provisional application Ser. No. 10 / 927,904, filed Aug. 26, 2004, which claims the benefit of the filing date of U.S. Provisional Appl. Ser. No. 60 / 514,423, filed Oct. 24, 2003 and to U.S. Provisional App. Ser. No. 60 / 560,752, filed on Aug. 29, 2003.DESCRIPTION OF THE TEXT FILE SUBMITTED ELECTRONICALLY[0002]The contents of the text file submitted electronically herewith are incorporated herein by reference in their entirety: A computer readable format copy of the Sequence Listing (filename: CYPR 028 04US SubSeqList_ST25.txt, date recorded: Apr. 7, 2009, file size 13 kilobytes).FIELD OF THE INVENTION[0003]This invention relates generally to medical genetics and, more specifically, to methods for optimizing clinical responsiveness to chemotherapy.BACKGROUND OF THE INVENTION[0004]Folate (folic acid) is a vitamin that is essential for the life-susta...

Claims

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Application Information

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Patent Type & Authority Applications(United States)
IPC IPC(8): C12Q1/68A61K31/525G01NG01N33/574
CPCC12Q1/6883C12Q2600/156Y10T436/24C12Q1/6876G01N33/574C12Q2600/106A61P19/02A61P29/00A61P35/00A61P37/00
Inventor DERVIEUX, THIERRYWALSH, MICHAEL
Owner CYPRESS BIOSCI
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