The results of this prospective, multicentre, randomized, open-label study will allow to determine whether bromocriptine on top of standard heart failure medication leads to improvement of LV function after 6 months in women with PPCM. In a very recent nationwide population-based study in the USA, the incidence and outcomes of PPCM were investigated in detail [3]. The authors demonstrated an increase of the incidence rate of PPCM, from 8.5 per 10,000 life births in 2011 to 11.8 per 10,000 life births in 2014. Importantly, the rate of maternal major adverse events defined as cardiac arrest, heart transplant, mechanical circulatory support, acute pulmonary edema, thromboembolism, or implantable cardioverter defibrillator/permanent pacemaker implantation increased from 11.7 % in 2004 to 15 % in 2011. Similar trends were observed for in-hospital mortality with an increase from 0.7 % in 2004 to 1.3 % in 2011. These data demonstrate that despite advances in medical care in Western societies during the last decade, the treatment concepts so far have failed to achieve improvements of the overall prognosis of PPCM patients. Therefore, with the rising incidence of PPCM and unaltered prognosis and lack of disease-specific therapeutics, there is an urgent need for novel therapeutic strategies [22]. This study is the first of this kind, and its results may contribute to the development of therapeutic strategies for the management of PPCM [3, 22].

The design of this study has been encouraged by a previous pilot study [12] and the findings of the non-randomized German PPCM registry [5] indicating beneficial effects of bromocriptine on LV function in PPCM. However, the current study is not fully comparable with the study be Sliwa et al. [12], which was placebo controlled as opposed to our study which compares low-dose short-term treatment of bromocriptine with prolonged bromocriptine treatment. This study design was based on ethical concerns about the continuation of lactation despite treatment of the patients with heart failure medication with potential side effects for the newborn, and because of the strong therapeutic effect of bromocriptine in the pilot study. Moreover, our ethic committee pointed out that stopping lactation without offering medical support is not allowed in Germany. The rationale for this treatment concept is based on experimental and clinical observations that a cleaved form of the nursing hormone prolactin, the 16 kDa prolactin, plays a causal role in the development of PPCM [9, 12]. This cleaved peptide exerts strong angiotoxic effects, in particular on the microvasculature, ultimately leading to cardiomyocyte cell death, and fibrosis. This hypothesis is supported by the evidence of increased serum levels of 16 kDa prolactin and augmented activity of the cleaving enzyme, cathepsin D [5, 12], at baseline in PPCM patients as compared to postpartal healthy women. Therefore, early pharmacological blockade of prolactin with bromocriptine may eliminate the detrimental effects of 16 kDa prolactin, prevent damage of the microvasculature, cell death, and replacement fibrosis, and thus, avoid adverse remodeling of the diseased myocardium and improve cardiac function and clinical condition of patients with acute onset of PPCM [9, 12]. Moreover, additional pleiotropic effects of bromocriptine are assumed to contribute to the healing process of the injured myocardium in PPCM. For example, proinflammatory pathways are known to be involved in the pathophysiology of PPCM [8, 23], which appear to be modulated upon treatment with bromocriptine [9, 23]. Further studies are warranted to identify precise mechanisms by which bromocriptine modulates the immunological responses that are activated in the development of PPCM. Other beneficial effects that have been attributed to bromocriptine are potential cytoprotective and antioxidative capabilities that could compensate for defective antioxidative mechanisms proposed as an important pathophysiological aspect in PPCM [8, 9]. Taken together, the cardioprotective effects of bromocriptine are broader than just effective prolactin blockade.

The basis of the dose and duration of bromocriptine therapy in the present trial were previous observations in animal models and case reports [11] which appeared to be efficient in the pilot bromocriptine study [12]. The change of LVEF was chosen as the primary endpoint as it is suitable for relatively small sample sizes of rare diseases such as PPCM.

Although blinding of the study is not possible due to ethical concerns, the data analysis and assessment of outcome is performed by blinded investigators which may partly compensate for the unavoidable open-label design.

To date, the observations obtained from this study indicate good safety and tolerability of bromocriptine in PPCM patients. So far, none of the patients had to prematurely terminate bromocriptine medication due to safety concerns. In particular, no bromocriptine-associated thrombotic complications were recorded. Only one patient experienced an adverse event in terms of temporary nausea.

In summary, this study addresses the potential of bromocriptine as add-on therapy in addition to standard heart failure therapy to improve LV function in acute PPCM. While initial results point to an adequate level of safety and tolerability, final follow-up evaluation of all planned patients need to be awaited to definitely determine the effect of bromocriptine on LV function in patients with acute PPCM. The results of this trial may have decisive impact on future management of PPCM patients.