Patients that were admitted to the University of Fukui Hospital between March 2011 and February 2013 were retrospectively evaluated in the present study. The study was approved by the ethics committee of University of Fukui Hospital, (Fukui, Japan). All patients had been diagnosed with hematological malignancies and already exhibited TLS or were at risk of TLS. These patients received rasburicase for the indicated durations, with or without the sequential administration of a xanthine oxidase inhibitor, either febuxostat or allopurinol, during induction chemotherapy. The patients did not receive any other medications that may have affected the S-UA level, which included losartan, fenofibrate, atorvastatin, pyrazinamide and cyclosporine.

The risk classification for TLS was made based on previously reported guidelines (2). Diseases at an intermediate risk for TLS consisted of acute myeloid leukemia with a peripheral white blood cell count between 1×10⁴ and 5×10⁴ cells/µl, acute lymphoblastic leukemia with a peripheral white blood cell count between 5×10⁴ and 1×10⁵ cells/µl, diffuse large B cell non-Hodgkin's lymphoma, and other hematological malignancies that would proliferate rapidly with expected rapid response to therapy (2). Diseases at a high risk included acute monoblastic leukemia, acute myeloid leukemia with a peripheral white blood cell count ≥5×10⁴ cells/µl, and acute lymphoblastic leukemia with a peripheral white blood cell count ≥1×10⁵ cells/µl (2). TLS is divided into laboratory TLS and clinical TLS. Laboratory TLS is defined according to abnormal serum values of UA, potassium, phosphate or calcium (1,2). Clinical TLS requires the presence of clinical manifestations, including increased creatinine levels, cardiac arrhythmia and seizure, in addition to laboratory TLS. The treatment algorithm was based on the aforementioned guidelines (2).

Hyperuricemia is broadly classified into UA-overproduction, UA-under-excretion and combined types, according to the guidelines for the management of hyperuricemia and gout that were published in Japan in 2010 (14). The urinary UA excretion, UA clearance and creatinine clearance rates were determined for the categorization of hyperuricemia. A urinary UA excretion rate of >0.51 mg/kg/h and a UA clearance rate of >7.3 ml/min was defined as overproduction type, a urinary UA excretion rate of <0.48 mg/kg/h or a UA clearance rate of <7.3 ml/min was classified as under-excretion type, and a UA excretion rate of >0.51 mg/kg/h and a UA clearance rate of <7.3 ml/min was classified as combined type.

All patients received rasburicase. The standard method of administration of rasburicase is 0.2 mg/kg/day for a maximum of seven days, which is covered by the national health insurance system in Japan. In the patients analyzed in the present study, the use of rasburicase was modified depending on the level of S-UA, according to the physicians' decision. Induction chemotherapy was initiated with a regimen suitable for each patient, alongside the administration of rasburicase. In certain cases, xanthine oxidase inhibitors, such as allopurol or febuxostat, were used in combination with the other agents. The primary endpoint was the normalization of the S-UA level to ≤7 mg/dl at the end of rasburicase treatment and on the seventh day subsequent to the first administration of rasburicase. The S-UA levels were determined at the University of Fukui Hospital using a TBA-c16000 automatic analyzer (Toshiba, Otawara, Tochigi, Japan) (15).

The total drug cost for treating TLS was calculated for each patient. Rasburicase (Rasritek; 7.5 mg) is priced at 49,938 yen in Japan, according to the standard price of these drugs determined by the Ministry of Health, Labour and Welfare in Japan, 2012. Febuxostat (Feburic™) at weights of 10, 20 and 40 mg costs 31.1, 56.4 and 106.6 yen, respectively. Allopurinol (Zyloric™) at a weight of 100 mg is 25.3 yen. If Rasritek is used in the standard regimen of 0.2 mg/kg/day for seven days, the total cost is 699,132 yen for an ordinary adult patient (60 kg).

All statistical analyses were performed using Microsoft Excel 2007 software (Microsoft, Redmond, WA, USA). All graphs were generated using GraphPad Prism software (version 5.0; GraphPad Software, Inc., San Diego, CA, USA). The data are reported as the mean ± standard deviation.

A total of 13 patients admitted to the University of Fukui Hospital between March 2011 and February 2013 were evaluated retrospectively (Table I). The median age was 67 years (range, 26–89 years), with eight males and five females. The diagnoses included diffuse large B-cell lymphoma (n=4), acute myeloid leukemia (n=7), acute lymphoblastic leukemia (n=1), and myelodysplastic syndrome (n=1). Patients 1, 3 and 6 already exhibited clinical TLS, while patients 3, 5, 7–9, 11 and 12 demonstrated laboratory TLS (Table I).

Eleven patients already presented hyperuricemia (patient numbers 1–3 and 5–12). The parameters associated with UA were determined in five patients (patients 1, 2, 8, 9 and 12), which included the urinary UA excretion and the UA clearance rates (Table II). On the basis of previously reported criteria (14), three cases were classified as UA overproducers and two cases were classified as UA under-excretors (Table II).

All patients underwent induction chemotherapy for the treatment of the diagnosed malignancies. Concomitantly, rasburicase was administered at various doses and durations (Table III). The median dose was 0.19 mg/kg, and the median duration was four days. Seven patients received rasburicase alone (patients 1, 5–8, 10 and 11), while six patients received rasburicase in combination with a xanthine oxidase inhibitor, either allopurinol (patients 2–4) or febuxostat (patients 9, 12 and 13) (Table III).

The primary estimate of the present retrospective study was the normalization of the S-UA level at the end of rasburicase treatment and on the seventh day subsequent to the first administration of rasburicase. While the S-UA baseline level was 10.4±4.5 mg/dl, the S-UA level at the end of rasburicase administration was 0.5±1.5 mg/dl (paired t-test; P<0.0001) and the S-UA level on day seven was 1.4±1.5 mg/dl (paired t-test, P<0.0001) (Fig. 1). All patients achieved the response criteria of normalization of the S-UA level. The patients were divided into two groups, a short-duration group, in which the patients received rasburicase for a maximum of three days, and a long-duration group, in which the patients received rasburicase for more than three days. The time course of S-UA was compared between these two groups (Fig. 2A and B). The S-UA level at baseline was 10.5±6.2 mg/dl for the short-duration group and 10.3±3.0 mg/dl for the long-duration group (P=0.47, Mann-Whitney test) (Fig. 2C). The S-UA level on day seven was 1.9±1.8 mg/dl for the short-duration group and 1.0±1.3 mg/dl for the long-duration group (P=0.20, Mann-Whitney test; Fig. 2D). This suggested that the S-UA level remained in the normal range in the short-duration group, although a non-significant re-increase in the S-UA level was observed.

Patient 10 received rasburicase treatment for seven days, and the S-UA level was completely suppressed (Fig. 3A). By contrast, patient 9 received two days of rasburicase treatment followed by the administration of febuxostat (Fig. 3B). In this case, despite the short duration of rasburicase use, sequential administration of febuxostat was suggested to suppress the S-UA level further (Fig. 3B). For the comparison between various dosages of rasburicase, patients five and eight received rasburicase for four days at the doses of 0.13 mg/kg and 0.22 mg/kg, respectively (Fig. 3C and D). These two cases clearly demonstrated an equivalent time course to achieving normalized S-UA levels (Fig. 3C and D), indicating that a smaller dose was equally effective for controlling S-UA production. Thus, the administration of rasburicase at smaller doses or for a shorter period of administration may be efficacious for managing the S-UA level in patients receiving chemotherapy with TLS or at risk of developing TLS. These results suggest that the method of administration of rasburicase may continue to require optimization.

The cost of drugs for treating TLS was calculated in each patient (Table II). When the cost for the standard regime of rasburicase treatment, consisting of 0.2 mg/kg/day for seven days, totaling 699,132 yen, was set as 100%, the mean real drug cost for treating TLS was 326,714 yen (range, 99,876–699,132 yen), or 47% (range, 14–100%), in all patients. This suggests that the cost for treating TLS largely depends on the use of rasburicase, regardless of the addition of allopurinol or febuxostat.