Direct Oral Anticoagulants (DOAC's)

Direct Oral Anticoagulants (DOAC's)
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Emad F. Aziz Cardiac Electrophysiologist Newark, New Jersey

Dr. Emad F. Aziz is a top Cardiac Electrophysiologist in New Jersey. With a passion for the field and an unwavering commitment to their specialty, Dr. Emad F. Aziz is an expert in changing the lives of their patients for the better. Through their designated cause and expertise in the field, Dr. Emad F. Aziz is a prime... more

The novel drugs are called dabigatran (Pradaxa), rivaroxaban (Xarelto), apixaban (Eliquis), and edoxaban (Lixiana). The trade names are those in parenthesis. Edoxaban was the most recent drug studied and was the subject of the Engage AF TIMI 48 trial (4).

First, your insurance provider might have a direct say into which drug you would take. One or two of these drugs may be approved for your use. 

In this regard, realize that all of these drugs are as good as, if not better, than warfarin for preventing stroke and all are better than warfarin in reducing your risk of serious bleeding in the brain. 

Some of these products are not reversible, similar to warfarin, and if you are bleeding the use of blood products and other measures may be required to help your body stop. 

However, there are some important differences to consider:

  1. Dabigatran (Pradaxa) was the first drug that was available in the United States. Dabigatran comes in two doses in the United States, 150 mg twice daily or 75 mg twice daily. Dabigatran was not only equal to warfarin, but it proved to be superior to it in preventing stroke in the RELY trial. Bleeding rates in the head were lower with dabigatran. However, bleeding from the stomach or bowels was higher. The most common side effect was dyspepsia, which is a term used to describe stomach pain. Dyspepsia was relatively common, occurring in approximately 11% of people. The lower dose available in the United States is for people that have moderate kidney dysfunction. It is important to know that the lower dose was not formally used in the RELY study.  Without a large body of clinical evidence to support the use of the lower dose and understand potential risks, I do not use it.
  2. Rivaroxaban (Xarelto) was the second drug available in the United States. Rivaroxaban comes in two doses, 20 mg daily or 15 mg daily. In the Rocket AF trial, rivaroxaban was at least as good and tended to be better than warfarin at preventing stroke. Rivaroxaban also significantly lowered the risk of bleeding in the brain and head. Bleeding in other locations was slightly higher with rivaroxaban compared to warfarin. The lower dose is for people that have moderate kidney dysfunction. This dose was actively studied in the trial and found to be both effective and safe.
  3. Apixaban (Eliquis) was the third drug to become available in the United States. Apixaban comes in two doses, 5 mg twice daily or 2.5 mg twice daily. In the Aristotle trial, apixaban was at least as good and tended to be better than warfarin at preventing stroke (3).  Similar to the other drugs, risk of bleeding in the brain and head was lower. However, this drug was unique in that bleeding from other sites including the stomach, bowels, and bladder was less. Overall, apixaban due to better efficacy and lower bleeding improved survival significantly compared to warfarin. Apixaban is the only drug that can claim that survival improved with its’ use compared to warfarin. The lower dose is for people that have moderate kidney dysfunction. This dose was actively studied in the Aristotle trial and found to be both effective and safe.
  4. Edoxaban (Lixiana) is not currently available in the United States. In the Engage AF TIMI 48 trial two doses were studied (60 mg and 30 mg daily) (4). This was a huge trial of 21,026 patients with follow-up of over 3 years in many patients. The higher dose of edoxaban was at least as good and tended to be better than warfarin at preventing stroke, however the lower dose was not as good as warfarin.  Cranial or head bleeding was better with both the higher and lower doses of edoxaban compared to warfarin. Bleeding from the stomach was greater than warfarin with the higher dose of edoxaban and lower than warfarin with the lower dose of edoxaban.

Which Drug Should I Take?

Here are a few things to consider with attached recommendations.

  1. If you have trouble taking drugs twice a day and often miss a dose, then you should use rivaroxaban or if it becomes available, the higher dose Edoxaban.  Unlike warfarin these drugs quickly leave your body. You have to be very compliant with the dosing schedule or you will be at higher risk for a stroke.
  2. If you have stomach pains or heart burn, then you should consider a drug other than dabigatran
  3. If you are most concerned about stroke and less worried about bleeding then dabigatran was the only drug that was superior (not equal or slightly better) than warfarin in preventing stroke
  4. If you are worried about bleeding or have experienced bleeding from the stomach, bowels, or bladder then apixaban is the better choice once you are cleared by your physician to use a blood thinner
  5. If you want the drug that will, because of both its’ benefits and risks, help you live longer compared to warfarin then apixaban is your choice
  6. If you have moderate kidney dysfunction then consider apixaban or rivaroxaban since these two drugs have reduced doses available that are well studied and found to be effective and safe
  7. If you have used warfarin for years and rarely if ever have to change your dose and you have not experienced adverse symptoms then continue your warfarin.

As mentioned before, all of these drugs reduce stroke at rates nearly equal or better than warfarin and all reduce brain bleed risk. For the first time in decades, warfarin has significant competitors that will help us as physicians prevent one of the most devastating complications with atrial fibrillation, stoke.