Javed Butler, MD, MPH

One of the signals we saw in RELAX-AHF, a trial of serelaxin in patients with acute HF, was preservation of kidney function in terms of cystatin-C levels. This study takes it to the next level in a more mechanistic way as we try to understand why serelaxin may have a beneficial effect on the kidneys. What we saw in this renal mechanistic study was a substantial improvement in renal plasma flow with the use of serelaxin over placebo. That does have the potential impact of improving kidney function in patients with acute HF, and that may translate into improved outcomes.

That it didn’t affect the GFR is a signal that the kidneys don’t have to work as hard. Although the GFR was maintained, the filtration fraction was reduced. As we know, there are a lot of intraglomerular hemodynamic changes that occur in patients with HF, and especially in acute HF, to increase filtration fraction in order to maintain the GFR. So the fact that filtration fraction went down and the GFR was maintained, related to increase in blood supply, suggests easing of the burden on the kidneys.

This field is incredibly important. For the past 20 years, when patients with acute HF come into the hospital, they have an approximately 30% chance of dying within 1 year. Unfortunately, many patients and providers may not fully appreciate this fact. Right now, we have not a single approved therapy for patients with acute HF that has been shown to reduce postdischarge mortality. So drugs like this and studies like this are critically important for us to understand and move the field forward. Hopefully, we can bend the curve.

Uri Elkayam, MD

Serelaxin is an exciting new drug and the results of the clinical trials are very promising. The beneficial effect of the drug is most probably related to its vasodilatory effect. The concept of vasodilation in HF makes great clinical sense. Drugs such as nesiritide (Natrecor, Scios) and nitroglycerin have a potent hemodynamic effect and definitely provide symptomatic improvement to individual patients. Unfortunately, for a variety of reasons, including drug dosing, timing of administration and heterogeneous patient population, nesiritide in the ASCEND-HF trial did not live up to expectations and failed to improve symptoms and outcome. Nitroglycerin, which is widely used, has never been evaluated properly and therefore many questions regarding its efficacy, including its effective dose and the impact of nitrate tolerance, as well as regarding its safety and side effects, still need to be answered in a large randomized trial.

Because of the above-mentioned limitations of existing vasodilators, the positive signals we’re getting from the studies of serelaxin in acute HF are really encouraging. This time, the dose of the drug was carefully selected; also, it was given early after hospitalization and to patients with preserved BP. The studies have shown a favorable side-effect profile, improvement of symptoms and even a positive effect on long-term outcomes. The effect on the kidney is an important part of the therapeutic effect or action of any drug used for this indication. Serelaxin was found to increase renal blood flow without a change in renal function or urinary volume. Though this is somewhat disappointing, and suggests that the renal effect of serelaxin is not the main cause for its beneficial clinical effects, at least the drug seems renal-friendly and it should not have any untoward renal effects.