Optimism and no longer foolishness? Haematology/oncology and the PICU

Theodore Roosevelt [1] said: “Optimism is a good characteristic but if carried to excess becomes foolishness.” Something similar—but less eloquent—might often have been said by a paediatric intensivist to a haematology/oncology colleague. Or worse: a senior colleague once asked: “Why do we put nails in coffin lids?” Before the punchline: “To stop the oncologists giving one more round of chemo.” This is clearly now (and was then) an absurd exaggeration. But perhaps what lies behind this tension is captured in Roosevelt’s [1] next line: “We are prone to speak of the resources of this country as inexhaustible. This is not so.” Neither are paediatric intensive care resources inexhaustible. Therefore, intensivists are used to balancing costs and benefits of aggressive or palliative treatment. We, consciously or unconsciously, ration our limited resources [2]. But could bad outcomes, such as those perceived for children with cancer, become a self-fulfilling prophecy with out-of-date risks informing plans to withdraw or withhold treatments? How do we avoid circular arguments wherein our perceptions of poor prognosis may contribute to poor outcomes in the plans we make with families or the intensity of the support we offer?

The answer is in large, systematically collected data sets. Many paediatric intensivists are aware that the paediatric index of mortality (PIM score) [3, 4]—now in its third full iteration (PIM3) [5]—describes a much higher PICU mortality for the same admission physiology amongst haematology/oncology cases than the general PICU population. The terms ‘leukaemia/lymphoma outside of first induction’ or ‘bone marrow transplant recipient’ both represent ‘very high-risk’ diagnoses. In 53,112 recent cases, either of these fields carries a fivefold greater risk of death with equivalent severity of organ failure at admission. This is the same tariff as a cardiac arrest preceding PICU admission [5].

This dismay-inducing comparison needs to be seen in the light of the knowledge of the haematologist/oncologist that many children with cancer (38 % at some point in their illness) will be admitted at to a PICU [6]. And they know that their meticulous cancer registry data show impressive and improving results. Five-year survival for a child with cancer is now at 83 % [7]. So for a haematologist/oncologist, PICU is a frequent stopover on a pathway to cure.

To try to understand and reconcile these differing assessments of risk and benefit, we must be precise in our descriptions of patients. Zinter et al. [8] have provided a description of outcomes for 10,365 paediatric cancer emergency admissions out of 246,346 admissions to the US virtual PICU systems database. The overall mortality was only 6.8 %. We should take note of this number. It is lower than most series quote for previously healthy children with community-acquired sepsis or acute respiratory distress syndrome (ARDS) on PICU [9‐12]. The observed relative risk of PICU death is still highly significant at 2.9 (95 % CI 2.7–3.1), but the truth is that this reflects the overall improvement in PICU outcomes more than cancer lagging behind. Indeed, if we compare the predicted risk of mortality for a child with sepsis-induced multiple organ dysfunction syndrome (MODS) or ARDS, with and without a high risk category of ‘leukaemia/lymphoma outside of first induction’ through each of the four published versions of the PIM scores since 1997, we see that the outcomes for cancer cases have been modelled as improving much faster than those of healthy children (Fig. 1). These results challenge us to understand the underlying mechanisms and to further refine and reflect on our practise. Similar trends have been observed in adult haematology and cancer [13]. It is unclear if the general improvements in ICU (e.g. early recognition and treatment of sepsis, or low tidal volume ventilation in ARDS) have been disproportionately effective in haematology/oncology cases. This is a credible explanation considering their higher baseline risk. Or does this arise from a specific therapy relevant to haematology/oncology? Certainly tumour lysis syndrome therapies are now highly effective. The change in mortality for adult cancer patients with ARDS is striking: 89 % mortality 1990–1995 vs. 52 % 2007–2011 [14]. This raises the possibility of a greater gain from more widespread use of non-invasive ventilation in this population [15, 16]. This hypothesis is currently under investigation in children (“SCARF” trial ISRCTN82853500) and adults (“IVNICTUS” trial NCT01915719).

There are more tantalising clues to the underlying mechanisms in Zinter et al.’s paper. Acute myeloid leukaemia was independently associated with high risk—consistent with recent work [17]. This might reflect the more immunosuppressive regimens. Certainly infection remains an independent risk factor. However, we know that the outcomes for neutropenic fever are now excellent (case fatality rate 0.7 %, 95 % CI 0.2–2.1) [18]. So perhaps these results also reflect toxicities of chemotherapy that matter more in the context of critical illness (e.g. cardiac toxicity of anthracyclines).

But we do not need speculation or further work, however, to recognise at least one important result in this paper: extracorporeal membrane oxygenation (ECMO) in haematology/oncology patients was associated with a 50 % survival (18/36 cases). This contrasts with the still dismal results for ECMO post haemopoietic stem cell transplantation [19]. Perhaps this is one directly relevant and clear distinction between optimism and foolishness?

Most in-hospital deaths occur following withdrawal of intensive care. This clinical decision-making process is now better informed by an increased understanding of epidemiology as presented by Zinter. Further enrichment is now required, describing patient pathways, mode of death, and underlying pathophysiology. To do this we need increased dialogue and sharing of data between haematology/oncology and PICU. This should not be difficult; after all we are two of the most successful, best-resourced and high profile paediatric specialties. Both have developed rapidly in the last 40 years and constitute a large proportion of the in-patient facilities, staff and resources in tertiary children’s hospitals. We share a preoccupation with infection and the immune response. Most importantly both specialities have seen dramatic and continuous improvements in outcome. Survival is now the expected outcome for a cancer diagnosis or an episode of critical illness in a child. Each has refined techniques (mechanical ventilation or bone marrow transplant conditioning) that have resulted in dramatic reductions in iatrogenic harm and improved survival. Each has huge (perhaps the largest?) impacts on child mortality. We frequently share patients. Work like that of Zinter and colleagues is essential to optimise this collaboration.