ESC Congress 2014 Hot Line Session: Favourable effect of Pradaxa® on kidney function over time compared to warfarin

RE-LY® sub-analysis shows that Pradaxa® treatment favourably affects kidney function[1] deterioration over time compared to warfarin
Data provide additional support for long-term use of Pradaxa® in stroke prevention in non-valvular atrial fibrillation (NVAF)[1]

September 03, 2014 10:35 Korea Standard Time

INGELHEIM, GERMANY--(Business Wire / Korea Newswire)--Non-US/Non-UK/Non-Canadian Media

New data presented today indicate that kidney function decline is less pronounced in patients with an irregular heartbeat (non-valvular atrial fibrillation, NVAF) who are treated with Pradaxa® (dabigatran etexilate) compared to warfarin.[1] A natural decline in kidney function is expected as part of the ageing process or as a result of other underlying diseases.[2] New data support that long-term Pradaxa® treatment compares favourably to warfarin in terms of kidney function decline over time.[1] The new RE-LY® study sub-analysis findings were presented today at a Clinical Trial Update Hot Line session during the ESC Congress 2014 organised by the European Society of Cardiology in Barcelona.[1]

“These data support dabigatran as a good long-term treatment option for non-valvular atrial fibrillation patients,” said Professor Michael Böhm, Director of the Department of Internal Medicine and Cardiology at the University Hospital of Saarland, Homburg/Saar, Germany. “These RE-LY® study findings may have particular relevance for NVAF patients who have co-existing medical conditions which negatively impact their kidney function, such as diabetes, and for patients with poorly controlled vitamin K antagonist therapy. Dabigatran may provide additional benefit to these patients in the long term.”

The data included in the ESC Congress 2014 Hot Line session were derived from a post hoc exploratory analysis of the RE-LY® study that included over 18,000 patients and compared kidney function change in patients treated with either warfarin or Pradaxa® (110mg or 150mg twice daily).[1]

Results indicate that kidney function deteriorated more in patients on warfarin compared to those on either dose of Pradaxa®.[1] Results were significantly different to warfarin for both doses of Pradaxa® at 30 months, with similar patterns seen in different Pradaxa® subgroups.[1] Patients who were poorly controlled on warfarin and spent more time above the recommended International Normalized Ratio target range (INR 2-3) experienced a markedly sharper decline in kidney function compared to patients taking Pradaxa®.[1] Patients with diabetes, who are at generally higher risk of kidney problems were particularly susceptible to the effects of warfarin, and experienced higher rates of kidney decline than non-diabetic NVAF patients.[1] The same was true for patients previously treated with warfarin.[1] Also in these patients, Pradaxa® treatment compared favourably to warfarin.[1]

While the exact mechanism behind this difference has yet to be identified, there is a well-defined pathophysiological background. Vitamin K is known to protect against the build-up of calcium deposits in blood vessels, known as vascular calcification.[3] Oral anticoagulation with vitamin K-antagonists such as warfarin, which block vitamin K in the body, have been associated with an increased rate of vascular calcification and vascular damage.[3] Pradaxa® is an oral direct thrombin inhibitor which does not interfere with vitamin K, but works in a different way to reduce blood clotting in order to protect patients with non-valvular atrial fibrillation against stroke.[4,5,6]

Please click on the link below for ‘Notes to Editors‘ and ‘References‘:

http://www.boehringer-ingelheim.com/news/news_releases/press_releases/2014/02_september_2014_dabigatranetexilate.html

Website: http://www.boehringer-ingelheim.com

Contact

Boehringer Ingelheim
Corporate Communications
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Friederike Middeke
55216 Ingelheim/Germany
Phone: +49 6132 – 77 141 575
Fax: +49 6132 – 77 6601

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