Abstract

Vitamin K antagonists are being used in the last five decades as an effective anticoagulant. However, for the past few years, new oral anticoagulants (NOACs) have been introduced as newer anticoagulant agents, which are gradually replacing the previously used vitamin K antagonist. Yet, these agents have not fully replaced the use of warfarin and heparin. NOACs have few advantages over the vitamin K antagonist as they act on a specific factor of coagulation cascade rather than inhibiting the whole vitamin K synthesis.In this article, all the data has been searched electronically on PubMed and PRISMA guidelines were not followed. Instead, we used MOOSE statements and the data searched on PubMed was from articles published in the last five years.A total of 12,269 patients were observed;,out of which 64.19% had active cancer and 35.80% was observed as a control group comprised of both male or female participants. Approximately 61.14% were using NOACs, 42.83% were on warfarin, and 2.72% were on low-molecular-weight heparin (LMWH). The NOACs used in different patients were in the following percentages; edoxaban (6.81%), apixaban (5.28%), dabigatran (10.09%), and rivaroxaban (10.02%).The use of NOACs has been increasing day by day but these agents have not completely replaced the warfarin or heparin, because of some demerits associated with the use of warfarin and some conditions where these drugs should be avoided. All NOACs have either hepatic or renal clearance so the hepatic activity and creatinine clearance rate must be monitored before the start of NOACs. The drug interaction between anticancer drugs and NOACs is still not fully reported.The effects of NOACs in AF and VTE are therapeutically effective, but in oncology patients several other co-factors are also involved with the use of NOACs due to which, it is either contraindicated or in some cases dose adjustment is required. However, very little information has been collected and more investigation must be done in this perspective.

Highlights

  • BackgroundAccording to Danny Hillis, “A human body is under continuous conversation, both within the cells and between the cells, and they coordinate with each other to grow and to die and when you are sick, something is gone wrong with that conversation”.Warfarin and heparin are being used for more than 50 years as anticoagulants; yet, we need to carefully monitor the effect of VKA to avoid bleeding and loss of efficacy [1]

  • The new oral anticoagulants (NOACs) used in different patients were in the following percentages; edoxaban (6.81%), apixaban (5.28%), dabigatran (10.09%), and rivaroxaban (10.02%)

  • All NOACs have either hepatic or renal clearance so the hepatic activity and creatinine clearance rate must be monitored before the start of NOACs

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Summary

Introduction

BackgroundAccording to Danny Hillis, “A human body is under continuous conversation, both within the cells and between the cells, and they coordinate with each other to grow and to die and when you are sick, something is gone wrong with that conversation”.Warfarin and heparin are being used for more than 50 years as anticoagulants; yet, we need to carefully monitor the effect of VKA to avoid bleeding and loss of efficacy [1]. According to Danny Hillis, “A human body is under continuous conversation, both within the cells and between the cells, and they coordinate with each other to grow and to die and when you are sick, something is gone wrong with that conversation”. New oral anticoagulants (NOACs) have several benefits over the previously used anticoagulants [2]. The advancement of ximelagatran has set the basis of “NOACs”. In the year 2003, ximelagatran was accepted in Europe for short-term venous thromboembolism as a direct oral anticoagulant. This drug was rejected and removed from the market because of the rise in liver enzymes due to this drug, but this set the basis for the advancement of NOACs [1]

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