Introduction
Oxaliplatin is a third-generation platinum
derivative that has been widely used in patients with
gastrointestinal malignancies, including colorectal cancer (CRC).
Results of a number of studies showed that the combination of
5-fluorouracil, leucovorin and oxaliplatin (FOLFOX) increased
survival rate and reduced the risk of disease progression in
patients with metastatic CRC and stage III colon cancer (1,2).
Thrombocytopenia has been noted in more than 70% of patients
receiving FOLFOX, but is usually self-limited and related to
myelosuppression from oxaliplatin (3,4). The
isolated and acute decline in platelets after FOLFOX treatment is
thought to be immune-mediated, and is referred to as drug-induced
immune thrombocytopenia (DIIT). Oxaliplatin-dependent antibody
against the platelet glycoprotein IIb/IIIa complex has been
identified in patients with oxaliplatin-induced immune
thrombocytopenia (5).
Drug-induced acute thrombocytopenia is an extremely
rare side effect that may occur immediately after oxaliplatin
infusion (3,4). This potentially fatal reaction is
immune-mediated and may be anticipated based on mild hemorrhagic
signs during previous administration. This is the first report of
acute thrombocytopenia occurring during adjuvant treatment of
colorectal cancer with oxaliplatin. Clinicians should be aware of
this adverse event to prevent possible serious consequences and
stop further oxaliplatin administration. Oxaliplatin is a
third-generation platinum agent that is active in the treatment of
colorectal adenocarcinoma. Drug-induced immune thrombocytopenia and
hemolytic anemia have been reported following the administration of
several compounds including cytotoxic agents and platinum
derivatives. Oxaliplatin is capable of inducing the formation of
drug-dependent antibodies that react with red blood cells or, less
frequently, thrombocytes. In the presence of sensitizing plasma
concentrations of oxaliplatin, these antibodies are able to mediate
the peripheral destruction of blood cells, leading to acute
hemolytic anemia, thrombocytopenia, or both (Evan’s syndrome)
(5). We report the case of a woman
who developed acute thrombocytopenia with hemorrhagic diathesis
during adjuvant treatment of colorectal adenocarcinoma with
oxaliplatin, 5-fluorouracil and leucovorin. The study was aprroved
by the ethics committee of the university, and patient consent was
obtained.
Case report
A 55-year-old woman without relevant comorbidities
underwent sigmoidectomy in August 2007 for stage III colon
adenocarcinoma. In September 2007, the patient started adjuvant
chemotherapy with oxaliplatin, 5-fluorouracil and leucovorin
(FOLFOX-4), which caused the development of grade 3 neurotoxicity
after the 11th administration. Prior to starting the last (12th)
course of chemotherapy, a complete blood cell count showed the
following values: neutrophils 1800/mm3, platelets
136,000/mm3, and hemoglobin 11.1 g/dl. A blood count
revealed that the platelet level had dropped to
35,000/mm3, with no significant changes in the
hemoglobin level. The D-dimer value increased to 1.2 mg/ml. The
direct antiglobulin test (DAT) was strongly positive, with slight
increases in lactate dehydrogenase (LDH=664 U/l) and reticulocytes
(2.9%), whereas no relevant abnormalities in bilirubin, haptoglobin
or complement factors (C3 and C4) were observed. The administration
of corticosteroids was begun. Since the blood cell count returned
to acceptable levels within four days (Fig. 1), bone marrow biopsy was not
performed. The patient was subsequently discharged and laboratory
test results remained in the normal range during follow-up.
Discussion
Patients treated with oxaliplatin may develop
allergic or idiosyncratic reactions and, rarely, hematological
emergencies (3–5). Few cases of immune-mediated hemolytic
anemia and/or thrombocytopenia due to repeated oxaliplatin
infusions have been reported in the literature. To the best of our
knowledge, there are 20 reports of oxaliplatin-mediated acute
thrombocytopenia during adjuvant treatment of colorectal cancer,
whereas several occurrences have been described in the metastatic
setting (3–13). Anemia and thrombocytopenia due to
bone marrow suppression are often observed during treatment with
platinum compounds (cisplatin, carboplatin or oxaliplatin).
Nevertheless, acute-onset hemolytic anemia rarely occurs
immediately after the administration of platinum salts, including
oxaliplatin (9). The mechanism of
hemolysis is immune-mediated, but remains controversial and is not
completely understood (10). Some
authors described a penicillin-like reaction due to the absorption
of oxaliplatin into the cell membrane of erythrocytes, with
consequent exposure of strongly immunogenic epitopes of surface
glycoproteins (11). This mechanism
leads to the formation of drug-dependent antibodies that mediate
the peripheral destruction of erythrocytes in the presence of the
sensitizing compound. It is likely that the repeated administration
of oxaliplatin is necessary to induce and maintain the
immune-mediated response in sensitized subjects (3). All the known case reports share a high
cumulative dose of oxaliplatin administered prior to the appearance
of the immune reaction (3).
Hemolysis may be associated with fever, chills and abdominal or
back pain, mimicking an allergic reaction pattern, which is
occasionally observed during oxaliplatin infusion. Corticosteroid
premedication suppresses the immune-mediated mechanism,
contributing to the underestimation of oxaliplatin-induced acute
hematological disorders (10).
We investigated 20 cases including that of the
present study (3–13). There were 7 male cases and 13 female
cases (Table I). The patients
ranged in age from 38 to 79 years old, with an average of 58 years
of age. Acute thrombocytopenia occurred between the 3rd course and
24th course of L-OHP administration, with the average number of
courses being 14.2. There were 14 cases in which symptoms were
observed during and after the 10th course. This result indicates
that the symptoms are more likely to develop with an increase in
the number of administrations. The symptoms were observed in the 12
h after administration in 11 cases (55%) and from 12 to 24 h after
administration in 2 cases (10%), with both of these time-frames
representing precipitous onset. As an initial symptom, bleeding
from a purple spot or port-site due to thrombocytopenia was
observed in many cases (60%).
 | Table IReview of 20 cases of
oxaliplatin-induced acute-onset thrombocytopenia and
hemorrhage. |
Table I
Review of 20 cases of
oxaliplatin-induced acute-onset thrombocytopenia and
hemorrhage.
| Case | Gender | Age | Course | Platelet count | Platelet (after) | Onset | Symptoms | Treatment | Result |
|---|
| 1 | M | 56 | N/K | 99000 | 6000 | 5 h | Purpura,
gingivorrhagia | Steroids,
transfusion | Recovery |
| 2 | M | 52 | 9 | 182000 | 17000 | 1 day | Bleeding | Transfusion | Recovery |
| 3 | F | 40 | 13 | 153000 | 80000 | 1 day | Back pain | No | Recovery |
| 4 | F | 70 | 19 | 432000 | 2000 | 4 h | Skin rash | Transfusion | Recovery |
| 5 | M | 60 | 14 | 143000 | 2000 | 1 h | Hematemesis | Transfusion | Recovery |
| 6 | F | 79 | 15 | 221000 | 5000 | 4 h | Bleeding,
purpura | Steroids,
transfusion | Recovery |
| 7 | F | 38 | 17 | 150000 | 13000 | 2 days | Abdominal pain,
petechial hemorrhages | Transfusion | Recovery |
| 8 | F | 55 | 10 | 136000 | 6000 | 24 h | Not mentioned | Transfusion | Recovery |
| 9 | F | 59 | 20 | 253000 | 5000 | 8 h | Purpura,
gingivorrhagia | Steroids,
transfusion | Recovery |
| 10 | M | 64 | 24 | 163000 | 4000 | 1 h | Back pain | Transfusion | Death |
| 11 | F | 57 | 11 | 89000 | 17000 | 17 h | Bleeding | Transfusion | Recovery |
| 12 | F | 50 | 15 | 119000 | 5000 | 7 h | Purpura,
gingivorrhagia | Steroids,
transfusion | Recovery |
| 13 | M | 48 | 21 | 94000 | 1000 | 7 h | Purpura | Steroids,
transfusion | Recovery |
| 14 | F | 59 | 12 | 151000 | 20000 | 1 day | Petechial
hemorrhages | Steroids,
transfusion | Recovery |
| 15 | M | 60 | 3 | 226000 | 4000 | 1 day | Petechial
hemorrhages, tongue hematoma | IVIG infusion | Recovery |
| 16 | F | 66 | 3 | 87000 | 66000 | 5–10 min | Skin rash | Steroids | Recovery |
| 17 | F | 55 | 13 | 136000 | 8000 | Immediately | Petechial
hemorrhages | Steroids | Recovery |
| 18 | M | 78 | 17 | 104000 | 15000 | 1.5 h | Coma | Steroids,
transfusion, G-CSF | Death |
| 19 | F | 66 | 25 | N/K | 22000 | 4 days | Fever up, general
fatigue | Transfusion, HD | Recovery |
| Our case | F | 55 | 9 | 135000 | 35000 | 2 days | Bleeding | Steroids,
transfusion | Recovery |
A recommended treatment for drug-induced
thrombocytopenia is to stop ingesting the drugs that are presumed
to be the cause. However, for serious thrombocytopenia associated
with mucosal bleeding, aggressive treatment is preferable (12). This type of treatment might include
platelet transfusion, adrenocortical steroid hormone
administration, hormone intravenous high-dose γ-globulin therapy or
plasma exchange therapy (Table I).
For case 4, since the platelet count was at an abnormally low level
of 0.1×10 μl, 10 units of platelet transfusion and steroid pulse
were carried out (Table I).
In terms of prognosis, 12 cases showed improvement,
but one case in which cerebral hernia developed due to cerebral
hemorrhage resulted in death six days later (Table I). In addition, in two cases, the
same regimen was carried out after improvement was noted prior to
thrombocytopenia occurring again. However, it was concluded that
the regimen needed to be changed if thrombocytopenia developed. A
sudden decrease in platelet levels, if not promptly recognized and
treated, may be life-threatening due to the risk of acute
hemorrhage. Furthermore, an immunohemolytic reaction may threaten
the life of the patient because of the possibility of severe anemia
and/or acute renal failure.
Female patients with advanced CRC and prior
oxaliplatin exposure are more likely to develop this consequence,
although it may also occur in male patients. Therefore, it is
imperative that patients be thoroughly examined for signs and
symptoms of bleeding with concurrent complete blood count
evaluation even after recovery from hypersensitivity symptoms.
Heightened vigilance and prompt testing may be useful in
recognizing the development of antibodies in patients with
religious objections to transfusion prior to the onset of severe
thrombocytopenia. Following the discontinuation of oxaliplatin,
patients often undergo concurrent platelet transfusion, if
indicated. Additional tests such as a peripheral blood smear
examination and direct antiglobulin test are also useful in the
assessment for Evan’s syndrome or hemolytic-uremic syndrome in the
case of worsening anemia or hemolysis. Patients with documented
oxaliplatin-induced acute thrombocytopenia should not be
re-challenged with oxaliplatin and should have oxaliplatin listed
as a drug to which they have an allergy.
In conclusion, clinicians should be aware of the
possibility of oxaliplatin-induced hematological emergencies during
the treatment of CRC patients to optimize supportive treatment and
avoid toxic mortality. Signs or symptoms such as epistaxis, even if
mild, should be taken into account during treatment with
oxaliplatin, as they may signal the subsequent development of
serious adverse events.
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