Pharmacogenomic biomarker information differences between drug labels in the United States and Hungary: implementation from medical practitioner view

Varnai, Reka; Szabó, István; Tarlós, Gréta; Szentpeteri, Laszlo Jozsef; Sı́k, Attila; Balogh, Sándor; Sipeky, Csilla

doi:10.1038/s41397-019-0123-z

Cited by 7 publications

(5 citation statements)

References 21 publications

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“…Overall, there appears to be a lack of consensus between the actionable PGx biomarker in the FDA‐PGx table and the CPIC/DPWG guidelines. The lack of consensus between the FDA‐PGx and the CPIC/DPWG guidelines or the drug labels in other countries have also been reported recently 30,34,35 . One of the reasons could be due to the statistical power in clinical studies with a limited number of patients, particularly in clinical trials with patients carrying low‐frequency variants before the drug approvals.…”

Section: Discussionmentioning

confidence: 96%

“…The lack of consensus between the FDA-PGx and the CPIC/DPWG guidelines or the drug labels in other countries have also been reported recently. 30,34,35 One of the reasons could be due to the statistical power in clinical studies with a limited number of patients, particularly in clinical trials with patients carrying low-frequency variants before the drug approvals. Over the last decade with advances in F I G U R E 5 Summary of pharmacogenetic/genomic biomarker classification in the US Food and Drug Administration-pharmacogenetic/genomic (FDA-PGx) table.…”

Section: Discussionmentioning

confidence: 99%

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A retrospective analysis of actionable pharmacogenetic/genomic biomarker language in FDA labels

Yamazaki

2021

Clinical Translational Sci

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The primary goal of precision medicine is to maximize the benefit-risk relationships for individual patients by delivering the right drug to the right patients at the right dose. To achieve this goal, it has become increasingly important to assess gene-drug interactions (GDI) in clinical settings. The U.S. Food and Drug Administration (FDA) periodically updates the table of pharmacogenetic/genomic (PGx) biomarkers in drug labeling on their website. As described herein, an effort was made to categorize various PGx biomarkers covered by the FDA-PGx table into certain groups. There were 2 major groups, oncology molecular targets (OMT) and drug-metabolizing enzymes and transporters (DMET), which constitute ~70% of all biomarkers (~33% and ~35%, respectively). These biomarkers were further classified whether their labeling languages could be actionable in clinical practice. For OMT biomarkers, ~70% of biomarkers are considered actionable in clinical practice as they are critical for the selection of appropriate drugs to individual patients. In contrast, ~30% of DMET biomarkers are considered actionable for the dose adjustments or alternative therapies in specific populations such as CYP2C19 and CYP2D6 poor metabolizers. In addition, the GDI results related to some of the other OMT and DMET biomarkers are considered to provide valuable information to clinicians. However, clinical GDI results on the other DMET biomarkers can possibly be used more effectively for dose recommendation. As the labels of some drugs already recommend the precise doses in specific populations, it will be desirable to have clear language for dose recommendation of other (or new) drugs if appropriate.

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Section: Discussionmentioning

confidence: 96%

Section: Discussionmentioning

confidence: 99%

A retrospective analysis of actionable pharmacogenetic/genomic biomarker language in FDA labels

Yamazaki

2021

Clinical Translational Sci

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“… 145 , 146 In certain fields in medicine such as oncology, due to high side-effect profile and astronomic costs of new biologic and chemotherapy medications, precision medicine is rapidly being implemented in clinical practice. 147 - 149 Despite the enormous cost of caring for transplant patients and vulnerability of these patients, transplant medicine is lagging behind in implementing precision prescribing. Therefore, in addition to potential optimization of transplant outcomes, precision medicine in kidney transplantation may be cost-effective from payer’s standpoint.…”

Section: Pharmacogenetics In Transplantationmentioning

confidence: 99%

Precision Medicine in Kidney Transplantation: Just Hype or a Realistic Hope?

Nobakht

Jagadeesan

Paul

et al. 2021

Transplantation Direct

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Abstract. Desirable outcomes including rejection- and infection-free kidney transplantation are not guaranteed despite current strategies for immunosuppression and using prophylactic antimicrobial medications. Graft survival depends on factors beyond human leukocyte antigen matching such as the level of immunosuppression, infections, and management of other comorbidities. Risk stratification of transplant patients based on predisposing genetic modifiers and applying precision pharmacotherapy may help improving the transplant outcomes. Unlike certain fields such as oncology in which consistent attempts are being carried out to move away from the “error and trial approach,” transplant medicine is lagging behind in implementing personalized immunosuppressive therapy. The need for maintaining a precarious balance between underimmunosuppression and overimmunosuppression coupled with adverse effects of medications calls for a gene-based guidance for precision pharmacotherapy in transplantation. Technologic advances in molecular genetics have led to increased accessibility of genetic tests at a reduced cost and have set the stage for widespread use of gene-based therapies in clinical care. Evidence-based guidelines available for precision pharmacotherapy have been proposed, including guidelines from Clinical Pharmacogenetics Implementation Consortium, the Pharmacogenomics Knowledge Base National Institute of General Medical Sciences of the National Institutes of Health, and the US Food and Drug Administration. In this review, we discuss the implications of pharmacogenetics and potential role for genetic variants-based risk stratification in kidney transplantation. A single score that provides overall genetic risk, a polygenic risk score, can be achieved by combining of allograft rejection/loss-associated variants carried by an individual and integrated into practice after clinical validation.

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“…The labeling for some of the products includes specific actions to be taken based on the genotype. In total, 28 drug label annotations already exist for psychiatric drugs, only in the field of oncology do more drug label annotations exist [ 1 ]. In psychiatry, the evidence for adverse drug events for certain genotypes is high as the therapeutic range is narrow in many antipsychotics and antidepressants.…”

Section: Introductionmentioning

confidence: 99%

Rates of Divergent Pharmacogenes in a Psychiatric Cohort of Inpatients with Depression—Arguments for Preemptive Testing

Roll

Hahn

2022

JoX

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Background: The international drug agencies annotate pharmacogenes for many years. Pharmacogenetic testing is thus far only established in few settings, assuming that only few patients are actually affected by drug-gene interactions. Methods: 108 hospitalized patients with major depressive disorder were genotyped for CYP1A2, CYP2B6, CYP2C8, CYP2C9, CYP2C19, CYP2D6, CYP3A4, CYP3A5, NAT2, DPYD; VKORC1 and TMTP. Results: We found 583 (mean 5.4, median 5) divergent phenotypes (i.e., divergent from the common phenotypes considered normal, e.g., extensive metabolizer) in the 12 analyzed pharmacokinetic genes. The rate for at least one divergent phenotype was 100% in our cohort for CYP, but also for all 12 important pharmacogenes: patients had at least two divergent phenotypes. Compared to a large Danish cohort, CYP2C9 NM and IM status, CYP2C19 UM, CYP2D6 UM and DYPD (GAS 0, 1, 2) genotypes differed statistical significantly. For CYP2D6 and CYP2C19, 13% of the patients were normal metabolizers for both enzymes in our cohort, but this value was 27.3% in the Danish cohort, which is a highly significant difference (p < 0.0001). Conclusion: Divergent phenotypes in pharmacogenes are not the exception, but the rule. Patients with divergent phenotypes seem more prone for hospitalization, emphasizing the need for pre-emptive testing to avoid inefficacy and adverse drug effects in all patients.

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Pharmacogenomic biomarker information differences between drug labels in the United States and Hungary: implementation from medical practitioner view

Cited by 7 publications

References 21 publications

A retrospective analysis of actionable pharmacogenetic/genomic biomarker language in FDA labels

A retrospective analysis of actionable pharmacogenetic/genomic biomarker language in FDA labels

Precision Medicine in Kidney Transplantation: Just Hype or a Realistic Hope?

Rates of Divergent Pharmacogenes in a Psychiatric Cohort of Inpatients with Depression—Arguments for Preemptive Testing

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