Genotype‐guided warfarin therapy: Still of only questionable value two decades on

What is known and objective Warfarin is an oral anticoagulant which has been widely used to treat and prevent thromboembolic events. Managing warfarin therapy requires careful monitoring and dose titration. This randomized controlled study was designed to assess the effect of genotype‐guided warfarin anticoagulation in Chinese elderly patients with nonvalvular atrial fibrillation. Methods 507 adults were randomized to receive initial dosing as determined by an algorithm containing genetic (VKORC1 and CYP2C9) plus clinical information or only clinical information. The primary endpoint was the time in therapeutic range (TTR) over 90 days. Secondary end points included haemorrhagic events, thrombotic events and mortality. Results The TTR was significantly different between genetic group and control group. The average TTR was (70.80 ± 24.39) % in the genotype‐guided group as compared with (53.44 ± 26.73) % in the control group. This represents a difference of 17.36% (95% CI, 11.82 to 22.89, P < .001). The cumulative incidence of total haemorrhagic events, minor haemorrhagic events, gastrointestinal bleeding and intracerebral bleeding events was not significantly different between two groups (P > .05). Follow‐up showed that the cumulative incidence of ischaemic stroke events occurred in the genetic group was significantly lower than that in the control group (2.39% vs 6.82%), and the genetic group had a significant lower risk than control group in cumulative incidence of ischaemic stroke events [HR 0.22, (95% CI 0.065 to 0.77), P < .05]. What is new and conclusion Genotype‐guided dosing could improve the average TTR, and follow‐up result showed that genotype‐guided therapy resulted in a significantly lower risk of ischaemic stroke events. Further research is required to focus on the clinical benefit of genotype‐guided dosing.

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“…But the clinical benefit of this is uncertain. Real‐world studies have not always corroborated trials‐based claims of clinical benefit 18 …”

Section: Discussionmentioning

confidence: 99%

Randomized controlled trial of genotype‐guided warfarin anticoagulation in Chinese elderly patients with nonvalvular atrial fibrillation

Zhu

Liu

2020

J Clin Pharm Ther

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“…In spite of largely accepted scientific evidence for PGx, some points of discussion still exist, most of which originate from the fact that, currently, PGx fails to explain 100% of variability in drug response. This could partly be explained by other factors affecting drug response, such as age, sex, co-medication, disease state, kidney and liver function, which may explain up to 60% of the interindividual variability in drug response [93]. In addition, our current understanding of PGx is still incomplete.…”

Section: Current Limitations Of Pgxmentioning

confidence: 99%

Potential of Whole-Genome Sequencing-Based Pharmacogenetic Profiling

et al. 2021

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Pharmacogenetics represents a major driver of precision medicine, promising individualized drug selection and dosing. Traditionally, pharmacogenetic profiling has been performed using targeted genotyping that focuses on common/known variants. Recently, whole-genome sequencing (WGS) is emerging as a more comprehensive short-read next-generation sequencing approach, enabling both gene diagnostics and pharmacogenetic profiling, including rare/novel variants, in a single assay. Using the example of the pharmacogene CYP2D6, we demonstrate the potential of WGS-based pharmacogenetic profiling as well as emphasize the limitations of short-read next-generation sequencing. In the near future, we envision a shift toward long-read sequencing as the predominant method for gene diagnostics and pharmacogenetic profiling, providing unprecedented data quality and improving patient care.

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“…More randomized clinical trials are needed for delineating the additional therapeutic benefit of CYP4F2 compared to CYP2C9 and VKORC1 combination. The result of this meta‐analysis needs to be interpreted with greater caution as the majority of the benefits observed with genotyping‐based strategies were in surrogate outcomes, and non‐genetic factors play a significant role in the inter‐individual response to warfarin 43…”

Section: What Is New and Conclusionmentioning

confidence: 99%

A network meta‐analysis ofCYP2C9,CYP2C9withVKORC1andCYP2C9withVKORC1andCYP4F2genotype‐based warfarin dosing strategies compared to traditional

Sridharan

Sivaramakrishnan

2020

J Clin Pharm Ther

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What is known and objectives: Variations in genotypes were observed in randomized clinical trials (RCTs) that evaluated genotype-based warfarin dosing. We carried out a network meta-analysis to assess whether any clinically significant differences exist between RCTs evaluating CYP2C9 with VKORC1, with CYP2C9 alone and CYP2C9, VKORC1, with CYP4F2 dosing strategies.Methods: Electronic records were searched for RCTs comparing genotype-based warfarin with traditional-dosing strategies. Key outcomes included were the time to first therapeutic international normalized ratio (INR); time to stable INR or warfarin dose; percent time in therapeutic range (TTR); and the proportion of patients with supra-therapeutic INR. Weighted mean differences (WMD) and odds ratios (OR) with 95% confidence intervals (95% CI) were the effect estimates.Results and discussion: Twenty-six studies (7898 patients) were included. CYP2C9based warfarin dosing was associated with a shorter time to first therapeutic INR (WMD: -2.73, 95% CI: -3.41, -2.05) and stable INR/warfarin dose (WMD: -8.1, 95% CI: -12.54, -3.66). CYP2C9 and VKORC1 were observed with a shorter time to first therapeutic INR (WMD: -1.92, 95% CI: -3.23, -0.61) and stable INR/warfarin dose (WMD: -4.6, 95% CI: -6.87, -2.34) along with a longer TTR (%) (WMD: 3.91, 95% CI:1.18, 6.63). CYP2C9, VKORC1 and CYP4F2 were observed with a reduced proportion of patients with supra-therapeutic INR (OR: 0.68, 95% CI: 0.49, 0.93). Trial sequential analysis confirms the superior benefits of CYP2C9 with VKORC1 genotype. What is new and conclusion:The present evidence is supportive of personalizing warfarin dose based only on CYP2C9 and VKORC1 genotypes compared to traditional strategies. More RCTs are needed to delineate any benefit for adding CYP4F2 to provide sufficient power for pooled analysis. No convincing evidence exists supporting the role of CYP2C9 alone.

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Genotype‐guided warfarin therapy: Still of only questionable value two decades on

Cited by 12 publications

References 202 publications

Randomized controlled trial of genotype‐guided warfarin anticoagulation in Chinese elderly patients with nonvalvular atrial fibrillation

Randomized controlled trial of genotype‐guided warfarin anticoagulation in Chinese elderly patients with nonvalvular atrial fibrillation

Potential of Whole-Genome Sequencing-Based Pharmacogenetic Profiling

A network meta‐analysis ofCYP2C9,CYP2C9withVKORC1andCYP2C9withVKORC1andCYP4F2genotype‐based warfarin dosing strategies compared to traditional

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