C. Lex et al., Infectious complications in children with acute lymphoblastic leukemia andT-cell lymphoma - a rationale for tailored supportive care, SUPP CARE C, 9(7), 2001, pp. 514-521
Infections still remain a major cause of therapy-associated morbidity and d
eath in patients with malignant diseases. To further lower the risk of seri
ous and long-lasting infections by additional supportive measures, detailed
information on the frequency and characteristic features of infections is
needed. Therefore, patient data from 112 children with acute lymphoblastic
leukemia and T-cell lymphoma who were treated according to the COALL-05-92
protocol in our department were analyzed for differences in the frequency a
nd origin of febrile episodes in relation to age, immunological type of leu
kemia, treatment in group assessed as being at high or low risk of relapse,
actual occurrence of relapse, and course of chemotherapy. At the time of d
iagnosis, low-risk patients more commonly presented with febrile episodes t
han high-risk patients. In total, patients developed a fever in 313 (24%) o
f 1,307 evaluated chemotherapy cycles. Febrile episodes were associated wit
h microbiologically or clinically documented infections in 60% of all cases
, while in 40% the fever was of unknown origin. Gram-positive pathogens had
a markedly higher incidence than gram-negative or fungal ones. The inciden
ce of febrile episodes during therapy appeared to be correlated with certai
n chemotherapeutic drug combinations. The highest rate was found after high
-dose cytarabine and asparaginase causing a long period of leukopenia. Howe
ver, after other chemotherapy courses with a similar duration of leukopenia
the incidence of febrile episodes was significantly lower, suggesting that
specific interactions of different chemotherapeutic agents with the immune
response might be an important factor in development of infections. Indivi
dual factors might also account for an increased incidence of infections, s
ince the number of highrisk patients with recurrent infections was signific
antly higher than expected on the basis of statistical evaluation. In concl
usion, our findings suggest that the risk of infections during chemotherapy
may not only be influenced by leukopenia, but that drug-specific effects o
f the various chemotherapeutic agents and individual factors may also be im
portant contributory factors. These observations must be further expanded i
n prospective studies so that new tailored supportive care protocols can be
elaborated.