(PRWEB) June 26, 2013

New Oral Anticoagulants Markets

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TriMarkPublications.com cites in its newly published New Oral Anticoagulants Markets report that the global anticoagulants market place will spike to over $ 24 billion by 2019.&#13

Anticoagulants decrease the capacity of the blood to create harmful blood clots that can in the end lead to a heart attack or stroke. Even though at times referred to as blood thinners, they do not truly thin the blood and only assist avoid the formation of new blood clots.

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Anticoagulants can be categorized into 5 major modalities: low molecular weight heparins (LMWHs), herapins, warfarin, direct thrombin inhibitors (DTIs) and element Xa inhibitors. For much more than 50 years and till not too long ago, the only oral anticoagulants have been vitamin K antagonists such as warfarin. Pradaxa (dabigatran), Xarelto (rivaroxaban), Eliquis (apixaban) and other new oral anticoagulants have a number of advantages over warfarin, including no periodical laboratory monitoring and far more predictable effects with fixed doses.

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The U.S. anticoagulants marketplace, which encompasses more than 60% of the worldwide industry for anticoagulants, will grow from $ 7.06 billion in 2012 to $ 15.32 billion in 2019 as it shifts from being monopolized by a single injectable anticoagulant, warfarin, to as soon as-daily oral anticoagulants.

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New Oral Anticoagulants Markets offers a thorough overview of these and other new oral anticoagulants, their authorized indications, drug profiles, pharmacokinetic parameters and the respective regions of marketplace growth.

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The report also examines businesses manufacturing anticoagulant equipment and supplies in the globe. Firms covered incorporate: Akers, Anthera, ARYx, AstraZeneca, Boehringer Ingelheim, Cipla, Daiichi Sankyo, Eisai, Eli Lilly, Genentech, GlaxoSmithKline, Medicines Business, Medicure, Merck, Novartis, Ortho-McNeil, Pfizer, Pharmion, Portola and Sanofi. Detailed charts with sales forecasts and marketshare data are incorporated.

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New Oral Anticoagulants Markets Table of Contents:

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1. Introduction &#13

1.1 Scope of this Report &#13

1.2 Methodology &#13

1.3 Executive Summary &#13

two. An Overview of Anticoagulants &#13

2.1 Scope of this Chapter &#13

2.1.1 Unmet Health-related Requirements with Existing Anticoagulants &#13

2.1.two Pharmacology of Injectable Anticoagulants &#13

2.1.3 Marketed and Registered Drugs for Anticoagulation and Related Disorders &#13

2.two Oral Anticoagulants &#13

two.two.1 Potential Limitations of New Oral Anticoagulants &#13

2.2.two Desired Attributes of Anticoagulants &#13

2.2.3 Comparison of New Anticoagulants &#13

two.2.four Bleed Rates of New Anticoagulants &#13

three. Selected Oral Anticoagulants &#13

3.1 Warfarin &#13

three.1.1 Warfarins Location in Clinical Therapy &#13

three.1.2 Drug Interaction with Warfarin &#13

3.1.3 Warfarins Interactions with Meals &#13

three.1.four Interactions of Warfarin with Dietary Vitamin K &#13

3.2 Dabigatran (Pradaxa) &#13

three.two.1 Use of Dabigatran in Particular Scenarios &#13

3.two.two Measuring the Anticoagulant Impact of Dabigatran &#13

three.2.three Activated Partial Thromboplastin Time (aPTT) &#13

3.two.four Thrombin Time (TT) and Hemoclot &#13

3.2.five Ecarin Clotting Time (ECT) &#13

three.two.six Prothrombin Time (PT) and INR &#13

three.two.7 Measures for Overdose &#13

three.2.8 Management of Bleeding Complications &#13

3.two.9 For Patients Undergoing Surgical Intervention &#13

3.two.ten For Dental Interventions &#13

three.2.11 For Spinal Anesthesia/Epidural Anesthesia/Lumbar Puncture &#13

3.2.12 For Individuals with Acute Coronary Syndrome (ACS) &#13

three.two.13 Cardioversion in Dabigatran Treated Individuals &#13

3.two.14 For Sufferers with Stroke &#13

three.two.15 Dabigatran right after Ischemic Stroke &#13

three.two.16 Strengths and Weaknesses of Dabigatran &#13

three.2.16.1 Strengths of Dabigatran in Metabolism, Pharmacokinetics and Pharmacodynamics &#13

3.two.16.two Weaknesses of Dabigatran in Metabolism, Pharmacokinetics and Pharmacodynamics &#13

three.two.16.three Strengths of Dabigatran in Laboratory Monitoring &#13

three.2.16.four Weaknesses of Dabigatran in Laboratory Monitoring &#13

three.2.16.5 Strengths of Dabigatran in Clinical Efficacy &#13

three.2.16.six Weaknesses of Dabigatran in Clinical Efficacy &#13

3.2.16.7 Strengths of Dabigatran in Controlling Bleeding &#13

three.two.17 Comparison of Dabigatran and Rivaroxaban in Sites of Action &#13

three.3 Rivaroxaban (Xarelto) &#13

three.3.1 Dosage and Administration &#13

3.three.2 Risk of Stroke right after Discontinuation in Non-Valvular Atrial Fibrillation &#13

3.three.three Threat of Bleeding &#13

3.3.4 Bleeding Events in ROCKET AF Trial &#13

3.three.5 Bleeding Events in RECORD Trial &#13

3.three.6 Overdosage &#13

3.three.7 Mechanism of Action &#13

3.three.8 Comparable Efficacy of Rivaroxaban &#13

three.three.9 Prophylaxis of Deep Vein Thrombosis &#13

three.four Eliquis (Apixaban) &#13

3.4.1 AVERROES Results &#13

3.5 Edoxaban &#13

3.six Betrixaban &#13

3.7 Pipeline Agents &#13

3.8 Comparison of Oral Anticoagulants &#13

three.9 Heparins &#13

3.10 Dalteparin (Fragmin) &#13

3.11 Enoxaparin (Lovenox) &#13

three.11.1 Indications and Usage &#13

3.11.2 Percutaneous Coronary Revascularization Procedures &#13

3.11.three Use of Lovenox with Concomitant Health-related Circumstances &#13

three.11.3.1 Thrombocytopenia &#13

three.11.three.2 Interchangeability with Other Heparins &#13

three.11.3.three Pregnant Ladies with Mechanical Prosthetic Heart Valves &#13

3.11.three.four Laboratory Tests &#13

three.11.three.5 Pharmacodynamics &#13

three.11.3.6 Pharmacokinetics &#13

three.12 Fondaparinux (Arixtra) &#13

3.13 Tinzaparin (Innohep) &#13

three.14 Semuloparin Sodium (AVE5026) &#13

3.15 Idrabiotaparinux &#13

three.16 Otamixaban &#13

three.17 RB006 &#13

three.18 Reversal Agents and Antidotes &#13

3.18.1 Vitamin K &#13

3.18.2 Recombinant Factor VIIa &#13

3.18.three Prothrombin Complex Concentrates &#13

four. A Short Overview of Antiplatelets &#13

four.1 Overview of this Chapter &#13

four.1.1 Differences between Antiplatelets and Anticoagulants &#13

4.1.2 Need to have for Antiplatelets &#13

four.1.3 Side Effects of Antiplatelets &#13

four.1.4 Selecting an Antiplatelet &#13

four.1.five Part of Platelets in Thrombosis &#13

four.1.6 Inhibitors of Platelet Adhesion &#13

4.1.7 Inhibitors of Platelet Activation &#13

four.1.7.1 Inhibitors of TXA2 Pathway &#13

four.1.7.two Inhibitors of P2Y12 &#13

four.1.7.three PAR-1 Inhibitors &#13

four.1.7.four Phosphodiesterase Inhibitors &#13

4.two Antiplatelet Drugs &#13

4.two.1 Aspirin &#13

four.two.2 Aggrenox &#13

four.two.3 Ticagrelor (Brilinta) &#13

four.2.4 Clopidogrel (Plavix) &#13

4.2.4.1 Indications and Usage &#13

4.two.four.2 Basic Risk of Bleeding &#13

four.two.5 Effient (Prasugrel) &#13

5. Coagulation Assays &#13

5.1 Clotting Assays &#13

five.1.1 Chromogenic Approaches &#13

5.1.2 Prothrombin Time &#13

5.1.three Activated Partial Thromboplastin Time &#13

5.1.4 Thrombin Time &#13

5.1.five Fibrinogen (Clauss Strategy) &#13

five.1.six Derived Fibrinogen &#13

5.1.7 Antithrombin &#13

five.1.eight Protein C &#13

five.1.9 Protein S &#13

five.1.10 Lupus Anticoagulants &#13

five.1.11 ProC International Assay and APC Resistance (APCR) &#13

5.two Influence of New Anticoagulants on Coagulation Assays &#13

6. Disease Conditions Targeted by Anticoagulants &#13

6.1 Cardiovascular Diseases &#13

6.1.1 Stroke &#13

6.1.2 Ischemic Stroke &#13

6.1.3 Hemorragic Stroke &#13

six.1.4 Subarachnoid Hemorrage &#13

six.1.five Worldwide Incidence and Prevalence of Stroke &#13

six.1.6 Incidence of Stroke in the U.S. &#13

six.1.7 Mortality from Heart Illness and Stroke i