Prognosis of AKI in malignant diseases with and without sepsis

The present investigation was a retrospective single-centre analysis. All patients treated at the medical intensive care unit of the department of nephrology and rheumatology (University Hospital of Göttingen, Germany) between 2009 and 2011 were included into the study. It was formally approved by the local ethics committee. Acute kidney injury was defined using the AKIN criteria [9]. Patients with pre-existing ESRD (end stage renal disease) were also included into the study. In these patients, any further acute aggravation of renal dysfunction was defined as AKI if the AKIN criteria were applicable and / or if, for other reasons, dialysis treatment was initiated. Indications for dialysis were the presence of one or more of the following criteria: refractory hyperkalemia, increases of serum creatinine >3 mg/dl and / or of blood urea nitrogen >100 mg/dl at any given time point, and signs / symptoms of fluid overload due to dimished urine output, respectively. As in earlier studies [10], sepsis was defined as systemic inflammatory response syndrome (SIRS) of infectious origin [11]. Thus, beside fulfilling the criteria of SIRS [12], all patients showed at least once positive blood cultures for either Gram-positive or Gram-negative bacteria and/or clinical symptoms of an infectous disease. The term malignancy was used in any case of tumor manifestation at the time of treatment at the ICU, regardless of the respective stage of the disease. Thereby, we differentiated between solid and non-solid (hemato-oncological) malignancies. For further clinical characterization a number of different parameters, such as c-reactive protein and the SAPS (Simplified Acute Physiology Score) II scores were documented on a daily basis. All data analyzed in this study were extracted from a database, belonging to the department of Nephrology & Rheumatology of the University Hospital of Göttingen.

All results are expressed as percentages. Differences between 3 or more groups were analyzed by ANOVA. Differences between two groups were analyzed by chi-square test. Significance was considered at p<0.05.

A total of 1.017 patients were included into the study. Six-hundred and eight were male, 409 were female, the mean age of all patients was 65 ±16 years with 65 ±14 years in men and 66 ±18 years in women. All patients were treated at the intensive care unit of the department of nephrology and rheumatology of the university hospital Göttingen (Germany) between 2009 and 2011. Sepsis was diagnosed in 330 patients (32% - 208 male [63%], 122 female [37%]), 687 patients (68%) did not fulfill the respective criteria. Two-hundred and twelve patients (21% - 138 male [65%], 74 female [35%]) suffered from a malignant disease at the time of admission to the ICU (non-solid tumor: 88, solid tumor: 124). Thirty-three patients with a non-solid tumor underwent bone marrow-/stem cell transplantation in their history. Four-hundred and thirty-five patients (43% - 278 male [64%], 157 female [36%]) either presented with AKI at the time of ICU admission or developed AKI during the treatment course at the ICU. Liver cirrhosis was diagnosed in 83 patients (8% - 57 male [69%], 25 female [31%]). The most important general outcome parameters of all included patients are summarized in Tables 1 and 2.

As pointed out earlier sepsis was diagnosed in 330 patients (32% - 208 male [63%], 122 female [37%]), 687 patients (68%) did not fulfill the respective criteria. In the no sepsis group 474 patients (69%) did not develop AKI while 213 (31%) presented with AKI of various severity. One-hundred and eight patients (32%) in the sepsis group did not suffer from AKI during the course of the disease, but AKI developed in 222 individuals (68%). Thus, AKI occured significantly more frequent in sepsis than in non-septic patients (p<0.001). The mortality rates within the respective groups were: no sepsis without AKI - 15% (72/474), no sepsis with AKI – 15% (31/213), sepsis without AKI – 36% (39/108), and sepsis with AKI – 53% (117/222). Mortality rates were significantly higher in patients with sepsis (± AKI) as compared to those without sepsis (± AKI). Additionally, patients with sepsis and AKI died more frequently than those wihtout AKI (Figure 1).

Two-hundred and twelve patients (21% - 138 male [65%], 74 female [35%]) suffered from a malignant disease at the time of admission to the ICU. A solid tumor was diagnosed in 123 patients (58%) while a non-solid tumor was apparent in 87 patients (42%). Incidences of AKI were: patients without malignancy 329/805 (41%), patients with a malignant disease (either solid or non-solid tumor) 104/212 (49%). The difference was statistically significant (p=0.032). Mortalty rates were: patients without tumor but with AKI 93/329 (28%), patients with malignancy and AKI 53/104 (51%). The calculated p-value was below 0.001. Thus, the coincidence of a malignant disease and AKI dramatically worsened the overall prognosis (Figure 2).

One-hundred and fifteen patients with a malignant disease did not suffer from sepsis (54% - 115/212). In this group, the incidence of AKI was 30% (35/115) and mortality was 22% (8/35). Ninety-seven patients with a malignancy were diagnosed with sepsis (46% - 97/212). In this particular group, AKI occurred in 69% (67/97), mortality was 67% (45/67). In both categories (incidence of AKI, mortality) differences between the two groups (tumor with vs. without sepsis) were significant (p-values lower than 0.001 - Figure 3). In a subgroup analysis, mortality rates of patients with sepsis and AKI were compared, depending on the presence of a solid versus non-solid tumor disease. As a matter of fact, patients with a non-solid tumor died in 100% if sepsis and AKI coincided, as compared to those with a solid tumor disease. In the latter group, mortality was 56% (p<0.001).

A total number of 341 patients required dialysis treatment. Subgroup analysis revealed the following frequencies of renal replacement therapy in patients with versus without malignant diseases: patients without tumor and without sepsis (28%) 94/341, mortality was 15% (14/94), patients without tumor but with sepsis (28%) 95/341, mortality was 46% (44/95), patients with tumor and without sepsis 6% (20/341), mortality was 20% (4/20), patients with tumor plus sepsis 11% (36/341), mortality was 66% (24/36). The following differences in mortality rates were statistically significant between the groups: no tumor, no sepsis versus no tumor, sepsis p<0.001, tumor, no sepsis versus tumor, sepsis p<0.001, no tumor, sepsis versus tumor, sepsis p=0.037.