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| Case Report | |
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Kirsty Wai Chung Leea, Kai Ming Chowa, c, Natalie Pui Ha Chanb, Angeline Oi Shan Loa, Cheuk Chun Szetoa
aDepartment
of Medicine & Therapeutics, bDepartment of Anatomical &
Cellular Pathology, Prince of Wales Hospital, The Chinese University of
Hong Kong, Shatin, Hong Kong, China Manuscript accepted for publication March 14, 2009 Running Title: Piperacillin/Tazobactam Induced Myelosuppression |
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| Abstract | |
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Key words: Piperacillin; TAazobactam; Myelosuppression; Neutropenia |
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| Introduction | |
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Case report |
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His haemoglobin level and platelet count recovered after stopping piperacillin/tazobactam. His empyema was subsequently treated with cefoperazon/sulbactam and gentamicin for another three weeks, with no further cytopenia observed.
Figure 1. Trend of (a) platelet count and (b) haemoglobin concentration in relation to piperacillin/tazobactam administration.
Figure 2. (a) Very hypocellular marrow aspirate at low power view; (b) Cellular area from the hypocellular bone marrow aspirate showing granulopoiesis with markedly reduced erythropoiesis. |
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| Discussion | |
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The mechanism by which marrow toxicity develops remains speculative. It is believed that piperacillin causes proliferation arrest of the myeloid cells. Only one case report of piperacillin/tazobactam related pancytopenia had been documented by bone marrow aspiration [2], which demonstrated a rich marrow with maturation arrest of all lineages. Moreover, published studies have also detected immunologically-mediated haemolytic anaemia and thrombocytopenia [1], in the presence of IgG antibodies against penicillins. Despite recent attention in the adverse haematological effects of piperacillin, current understanding is by and large derived from sporadic case reports pertaining to leucopenia [3-5], anaemia or thrombocytopenia [5-8]. More large-scale cohort studies suggested that the myelotoxicity is related to large cumulative doses. The adverse haematological reaction rarely occurs with treatment less than 10 days, although a study of 41 patients receiving piperacillin/tazobactam for bone-related infections showed no significant difference between the mean treatment duration of neutropenic and non-neutropenic patients [3]. The same study demonstrated a significantly younger mean age for the group with neutropenia. Younger patients, especially children, tend to be more vulnerable. Of the three published case reports regarding this topic, the patients were between the ages of 18 to 27 years [2, 6, 7]. In a case series of 25 patients, including five subjects under the age of 18, piperacillin was used to treat Pseudomonas infection. Six patients subsequently developed neutropenia, of which four were children [5]. Children appear to develop haematological toxicity with a shorter duration of piperacillin therapy when compared to adults. One case report has suggested that this effect may be related to body weight [2], and recommends a dosage reduction in underweight patients. Although piperacillin/tazobactam is eliminated in the urine, patients with renal insufficiency receiving dose-adjusted piperacillin/tazobactam therapy have not been reported to be at increased risk of myelotoxicity. Nevertheless, the delayed recovery of pancytopenia in our patient may well be explained by underlying renal failure, as well as the presence of hypocellular marrow, both of which have been found to be adverse prognostic factors for recovery in toxic neutropenia [9]. The true incidence of piperacillin bone marrow suppression is hitherto unknown, and may be explained by a paucity of data involving more than two weeks of piperacillin/tazobactam therapy. Much less is known about the genetic predisposition to this haematological adverse reaction of piperacillin/tazobactam. Further studies will also be critical in determining whether and, if so, which signal heralds the development of bone marrow suppression after piperacillin/tazobactam. The key points from this case are: Piperacillin/tazobactam treatment, if prolonged, can be associated with bone marrow suppression; Besides the oft-quoted neutropenia, other manifestation includes thrombocytopenia and/or pancytopenia; Vigilance by clinicians in detecting and diagnosing this reversible adverse drug reaction is important; Early recognition should probably be achieved by regular monitoring of blood counts in patients receiving more than 10 days of piperacillin/tazobactam. In conclusion, cytopenia involving any of the myeloid lineages may occur with prolonged piperacillin/tazobactam treatment. It would be wise to recommend, pending further evidence on this haematological adverse reaction of piperacillin, regular monitoring of blood counts in patients receiving more than 10 days of therapy. |
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| Footnotes | |
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| References | |
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| 1. |
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Digital Object Identifier (DOI):10.4021/jocmr2009.03.1227
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