A pharmacogenetic versus a clinical algorithm for warfarin dosing

Stephen E. Kimmel; Benjamin French; Scott E. Kasner; Julie A. Johnson; Jeffrey L. Anderson; Brian F. Gage; Yves D. Rosenberg; Charles S. Eby; Rosemary A. Madigan; Robert B. McBane; Sherif Z. Abdel-Rahman; Scott M. Stevens; Steven Yale; Emile R. Mohler; Margaret C. Fang; Vinay Shah; Richard B. Horenstein; Nita A. Limdi; James A.S. Muldowney; Jaspal S Gujral; Patrice Delafontaine; Robert J. Desnick; Thomas L. Ortel; Henny H. Billett; Robert C. Pendleton; Nancy L. Geller; Jonathan L. Halperin; Samuel Z. Goldhaber; Michael D. Caldwell; Robert M. Califf; Jonas H. Ellenberg

doi:10.1056/NEJMoa1310669

A pharmacogenetic versus a clinical algorithm for warfarin dosing

Stephen E. Kimmel, Benjamin French, Scott E. Kasner, Julie A. Johnson, Jeffrey L. Anderson, Brian F. Gage, Yves D. Rosenberg, Charles S. Eby, Rosemary A. Madigan, Robert B. McBane, Sherif Z. Abdel-Rahman, Scott M. Stevens, Steven Yale, Emile R. Mohler, Margaret C. Fang, Vinay Shah, Richard B. Horenstein, Nita A. Limdi, James A.S. Muldowney, Jaspal S GujralPatrice Delafontaine, Robert J. Desnick, Thomas L. Ortel, Henny H. Billett, Robert C. Pendleton, Nancy L. Geller, Jonathan L. Halperin, Samuel Z. Goldhaber, Michael D. Caldwell, Robert M. Califf, Jonas H. Ellenberg

General Internal Medicine

Research output: Contribution to journal › Article › peer-review

641 Scopus citations

Abstract

BACKGROUND: The clinical utility of genotype-guided (pharmacogenetically based) dosing of warfarin has been tested only in small clinical trials or observational studies, with equivocal results. METHODS: We randomly assigned 1015 patients to receive doses of warfarin during the first 5 days of therapy that were determined according to a dosing algorithm that included both clinical variables and genotype data or to one that included clinical variables only. All patients and clinicians were unaware of the dose of warfarin during the first 4 weeks of therapy. The primary outcome was the percentage of time that the international normalized ratio (INR) was in the therapeutic range from day 4 or 5 through day 28 of therapy. RESULTS: At 4 weeks, the mean percentage of time in the therapeutic range was 45.2% in the genotype-guided group and 45.4% in the clinically guided group (adjusted mean difference, [genotype-guided group minus clinically guided group], -0.2; 95% confidence interval, -3.4 to 3.1; P=0.91). There also was no significant between-group difference among patients with a predicted dose difference between the two algorithms of 1 mg per day or more. There was, however, a significant interaction between dosing strategy and race (P=0.003). Among black patients, the mean percentage of time in the therapeutic range was less in the genotype-guided group than in the clinically guided group. The rates of the combined outcome of any INR of 4 or more, major bleeding, or thromboembolism did not differ significantly according to dosing strategy. CONCLUSIONS: Genotype-guided dosing of warfarin did not improve anticoagulation control during the first 4 weeks of therapy.

Original language	English (US)
Pages (from-to)	2283-2293
Number of pages	11
Journal	New England Journal of Medicine
Volume	369
Issue number	24
DOIs	https://doi.org/10.1056/NEJMoa1310669
State	Published - 2013

ASJC Scopus subject areas

General Medicine

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Kimmel, S. E., French, B., Kasner, S. E., Johnson, J. A., Anderson, J. L., Gage, B. F., Rosenberg, Y. D., Eby, C. S., Madigan, R. A., McBane, R. B., Abdel-Rahman, S. Z., Stevens, S. M., Yale, S., Mohler, E. R., Fang, M. C., Shah, V., Horenstein, R. B., Limdi, N. A., Muldowney, J. A. S., ... Ellenberg, J. H. (2013). A pharmacogenetic versus a clinical algorithm for warfarin dosing. New England Journal of Medicine, 369(24), 2283-2293. https://doi.org/10.1056/NEJMoa1310669

Kimmel, SE, French, B, Kasner, SE, Johnson, JA, Anderson, JL, Gage, BF, Rosenberg, YD, Eby, CS, Madigan, RA, McBane, RB, Abdel-Rahman, SZ, Stevens, SM, Yale, S, Mohler, ER, Fang, MC, Shah, V, Horenstein, RB, Limdi, NA, Muldowney, JAS, Gujral, JS, Delafontaine, P, Desnick, RJ, Ortel, TL, Billett, HH, Pendleton, RC, Geller, NL, Halperin, JL, Goldhaber, SZ, Caldwell, MD, Califf, RM & Ellenberg, JH 2013, 'A pharmacogenetic versus a clinical algorithm for warfarin dosing', New England Journal of Medicine, vol. 369, no. 24, pp. 2283-2293. https://doi.org/10.1056/NEJMoa1310669

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title = "A pharmacogenetic versus a clinical algorithm for warfarin dosing",

abstract = "BACKGROUND: The clinical utility of genotype-guided (pharmacogenetically based) dosing of warfarin has been tested only in small clinical trials or observational studies, with equivocal results. METHODS: We randomly assigned 1015 patients to receive doses of warfarin during the first 5 days of therapy that were determined according to a dosing algorithm that included both clinical variables and genotype data or to one that included clinical variables only. All patients and clinicians were unaware of the dose of warfarin during the first 4 weeks of therapy. The primary outcome was the percentage of time that the international normalized ratio (INR) was in the therapeutic range from day 4 or 5 through day 28 of therapy. RESULTS: At 4 weeks, the mean percentage of time in the therapeutic range was 45.2% in the genotype-guided group and 45.4% in the clinically guided group (adjusted mean difference, [genotype-guided group minus clinically guided group], -0.2; 95% confidence interval, -3.4 to 3.1; P=0.91). There also was no significant between-group difference among patients with a predicted dose difference between the two algorithms of 1 mg per day or more. There was, however, a significant interaction between dosing strategy and race (P=0.003). Among black patients, the mean percentage of time in the therapeutic range was less in the genotype-guided group than in the clinically guided group. The rates of the combined outcome of any INR of 4 or more, major bleeding, or thromboembolism did not differ significantly according to dosing strategy. CONCLUSIONS: Genotype-guided dosing of warfarin did not improve anticoagulation control during the first 4 weeks of therapy.",

author = "Kimmel, {Stephen E.} and Benjamin French and Kasner, {Scott E.} and Johnson, {Julie A.} and Anderson, {Jeffrey L.} and Gage, {Brian F.} and Rosenberg, {Yves D.} and Eby, {Charles S.} and Madigan, {Rosemary A.} and McBane, {Robert B.} and Abdel-Rahman, {Sherif Z.} and Stevens, {Scott M.} and Steven Yale and Mohler, {Emile R.} and Fang, {Margaret C.} and Vinay Shah and Horenstein, {Richard B.} and Limdi, {Nita A.} and Muldowney, {James A.S.} and Gujral, {Jaspal S} and Patrice Delafontaine and Desnick, {Robert J.} and Ortel, {Thomas L.} and Billett, {Henny H.} and Pendleton, {Robert C.} and Geller, {Nancy L.} and Halperin, {Jonathan L.} and Goldhaber, {Samuel Z.} and Caldwell, {Michael D.} and Califf, {Robert M.} and Ellenberg, {Jonas H.}",

year = "2013",

doi = "10.1056/NEJMoa1310669",

language = "English (US)",

volume = "369",

pages = "2283--2293",

journal = "New England Journal of Medicine",

issn = "0028-4793",

publisher = "Massachussetts Medical Society",

number = "24",

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TY - JOUR

T1 - A pharmacogenetic versus a clinical algorithm for warfarin dosing

AU - Kimmel, Stephen E.

AU - French, Benjamin

AU - Kasner, Scott E.

AU - Johnson, Julie A.

AU - Anderson, Jeffrey L.

AU - Gage, Brian F.

AU - Rosenberg, Yves D.

AU - Eby, Charles S.

AU - Madigan, Rosemary A.

AU - McBane, Robert B.

AU - Abdel-Rahman, Sherif Z.

AU - Stevens, Scott M.

AU - Yale, Steven

AU - Mohler, Emile R.

AU - Fang, Margaret C.

AU - Shah, Vinay

AU - Horenstein, Richard B.

AU - Limdi, Nita A.

AU - Muldowney, James A.S.

AU - Gujral, Jaspal S

AU - Delafontaine, Patrice

AU - Desnick, Robert J.

AU - Ortel, Thomas L.

AU - Billett, Henny H.

AU - Pendleton, Robert C.

AU - Geller, Nancy L.

AU - Halperin, Jonathan L.

AU - Goldhaber, Samuel Z.

AU - Caldwell, Michael D.

AU - Califf, Robert M.

AU - Ellenberg, Jonas H.

PY - 2013

Y1 - 2013

N2 - BACKGROUND: The clinical utility of genotype-guided (pharmacogenetically based) dosing of warfarin has been tested only in small clinical trials or observational studies, with equivocal results. METHODS: We randomly assigned 1015 patients to receive doses of warfarin during the first 5 days of therapy that were determined according to a dosing algorithm that included both clinical variables and genotype data or to one that included clinical variables only. All patients and clinicians were unaware of the dose of warfarin during the first 4 weeks of therapy. The primary outcome was the percentage of time that the international normalized ratio (INR) was in the therapeutic range from day 4 or 5 through day 28 of therapy. RESULTS: At 4 weeks, the mean percentage of time in the therapeutic range was 45.2% in the genotype-guided group and 45.4% in the clinically guided group (adjusted mean difference, [genotype-guided group minus clinically guided group], -0.2; 95% confidence interval, -3.4 to 3.1; P=0.91). There also was no significant between-group difference among patients with a predicted dose difference between the two algorithms of 1 mg per day or more. There was, however, a significant interaction between dosing strategy and race (P=0.003). Among black patients, the mean percentage of time in the therapeutic range was less in the genotype-guided group than in the clinically guided group. The rates of the combined outcome of any INR of 4 or more, major bleeding, or thromboembolism did not differ significantly according to dosing strategy. CONCLUSIONS: Genotype-guided dosing of warfarin did not improve anticoagulation control during the first 4 weeks of therapy.

AB - BACKGROUND: The clinical utility of genotype-guided (pharmacogenetically based) dosing of warfarin has been tested only in small clinical trials or observational studies, with equivocal results. METHODS: We randomly assigned 1015 patients to receive doses of warfarin during the first 5 days of therapy that were determined according to a dosing algorithm that included both clinical variables and genotype data or to one that included clinical variables only. All patients and clinicians were unaware of the dose of warfarin during the first 4 weeks of therapy. The primary outcome was the percentage of time that the international normalized ratio (INR) was in the therapeutic range from day 4 or 5 through day 28 of therapy. RESULTS: At 4 weeks, the mean percentage of time in the therapeutic range was 45.2% in the genotype-guided group and 45.4% in the clinically guided group (adjusted mean difference, [genotype-guided group minus clinically guided group], -0.2; 95% confidence interval, -3.4 to 3.1; P=0.91). There also was no significant between-group difference among patients with a predicted dose difference between the two algorithms of 1 mg per day or more. There was, however, a significant interaction between dosing strategy and race (P=0.003). Among black patients, the mean percentage of time in the therapeutic range was less in the genotype-guided group than in the clinically guided group. The rates of the combined outcome of any INR of 4 or more, major bleeding, or thromboembolism did not differ significantly according to dosing strategy. CONCLUSIONS: Genotype-guided dosing of warfarin did not improve anticoagulation control during the first 4 weeks of therapy.

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DO - 10.1056/NEJMoa1310669

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SN - 0028-4793

VL - 369

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JO - New England Journal of Medicine

JF - New England Journal of Medicine

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A pharmacogenetic versus a clinical algorithm for warfarin dosing

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