Platinum-containing cytostatic drugs

Presentation

In about 90% of patients, oxaliplatin is associated with acute neurosensory toxicity, including dysesthesia and paresthesia. Neurosensory toxicity affects the fingers, toes, perioral and oral regions, and the pharyngolaryngeal tract (in about 1–2% of cases), which is generally induced or aggravated by coldness. As a result, patients should be instructed to avoid exposure to cold. Such symptoms can occur during or shortly after the first course of oxaliplatin. The symptoms are commonly mild and disappear within a few hours or days. Some patients also develop muscle cramps or spasms. The risk of acute neuropathy appears to be lower if oxaliplatin is given in a dosage of 85 mg/m ² every 2 weeks rather than 130 mg/m ² every 3 weeks. A further strategy to reduce the risk of acute recurrent pseudolaryngospasm is to increase the infusion duration from 2 to 6 hours during subsequent cycles [ , ]. The prophylactic use of infusions containing calcium and magnesium sulfate before and after oxaliplatin can prevent acute neurotoxic symptoms [ ].

• A woman developed bilateral blindness and lumbosacral myelopathy within 1 month of having received an autologous bone marrow transplant, cisplatin 55 mg/m ² , carmustine 600 mg/m ² , and cyclophosphamide 1875 mg/m ² [ ].

In addition to the acute neurotoxic symptoms caused by oxaliplatin, about 10–15% of patients develop a moderate neuropathy, particularly after cumulative intravenous doses of 700–800 mg/m ² . The symptoms of cumulative neuropathy include non-cold-related dysesthesia, paresthesia, superficial and deep sensory loss, and eventually sensory ataxia and functional impairment, which persists between treatment cycles. Most of these symptoms usually resolve a few weeks or months after oxaliplatin withdrawal. Lower cumulative doses (for example 510–765 mg/m ² ) and higher cumulative doses exceeding 1020 mg/m ² have been associated with incidences of cumulative grade 3 neurotoxicity of 3.2% and 50% respectively [ , , , ]. In addition, higher cumulative doses, exceeding 1000 mg/m ² , have been associated with severe, atypical neurotoxic symptoms, such as micturition disturbances and Lhermitte’s sign, mimicking cord disease. However, these signs have been observed in only a few patients so far (3.3% in phase 3 trials). Both symptoms appear to be reversible after oxaliplatin withdrawal [ ]. In some patients oxaliplatin treatment is feasible for as long as 18 months (for example cumulative oxaliplatin dose over 3000 mg/m ² ) with no signs of dysesthesia or paresthesia causing functional impairment, indicating high interindividual variability with respect to sensitivity to oxaliplatin-induced cumulative neuropathy [ , ]. Whether cumulative sensory neuropathy can occur as a result of accumulation of dichloro-DACH-platinum, a biotransformation product of DACH-platinum, in the axonal and dorsal root ganglia neurons, needs further investigation [ ].

Persistent Lhermitte’s sign (an electric-like sensation induced by flexion of the neck) suggestive of irreversible spinal cord toxicity has been reported in a patient taking cisplatin and etoposide [ ]. Of four patients with oxaliplatin neurotoxicity, two presented with Lhermitte’s sign, one had urinary retention, and one had both [ ]. All had received cumulative doses of 1248–2040 mg/m ² , which is more than the generally accepted neurotoxic threshold for oxaliplatin (1000 mg/m ² ).

Peripheral paresthesia has been reported 5 years after adjuvant cisplatin-based treatment for stages I and II testicular cancer [ ].

Four of eight children developed acute neurological toxicity. Three had seizures and one had transient blindness after high-dose cisplatin (200 mg/m ² ) given by continuous infusion over 5 days, followed 10 days later by a further 2 days with 40 mg/m ² /day. These children had the greatest deterioration in renal function, and they may have had impaired clearance of and increased exposure to cisplatin [ ].

Peripheral neuropathy with clinical signs and/or symptoms was found in 80% of patients who had received a cumulative dose of 576 mg/m ² of cisplatin. There was a dose-related reduction in sensory action potential amplitudes [ ]. The clinical and neurophysiological time progression of the severity of cisplatin polyneuropathy during and after treatment with cisplatin up to a cumulative dose of 600 mg/m ² has been described [ ].

The paraneoplastic neuropathy experienced by women with epithelial ovarian cancer receiving cisplatin has been attributed in certain cases to the drug [ ].

• A woman with cancer of the ovary and a man with oat cell carcinoma both developed paresthesia of all four limbs, reduced control of fine movements, and unstable gait after receiving a cumulative dose of 500 mg/m ² of cisplatin [ ]. There was distal hypesthesia, with conservation of temperature and pain sensation, areflexia, and sensory ataxia. The woman also had continuous pseudoathetosis. Neurophysiological studies showed absence of peripheral and central sensory potentials and of H-reflexes, normal electromyography, normal motor conduction, and normal mixed silent period.

The target organ in cisplatin neurotoxicity is the dorsal root ganglion. This patient had a syndrome that clinically and neurophysiologically suggested diffuse neuropathic involvement of the dorsal ganglion, in which absence of sensory and H-reflex potentials showed that the small myelinic cells were not altered, consistent with the preservation of pain and temperature sensation.

• A woman developed bilateral blindness and lumbosacral myelopathy within 1 month of having received an autologous bone marrow transplant, cisplatin 55 mg/m ² ,carmustine 600 mg/m ² , and cyclophosphamide1875 mg/m ² [ ].

Encephalopathy has also been reported.

• A 50-year-old woman with carcinoma of the cervix was treated with radiotherapy and six courses of cisplatin (75 mg/m ² every 3 weeks; total dose 810 mg) [ ]. The therapy was completed with no obvious acute complications, but 12 weeks after the last course, she developed sudden blindness associated with occipital headache. She had mild global cognitive deficits and intermittent myoclonic jerking of both arms. Her visual acuity was limited to light perception in both eyes; her pupils were symmetrical with no afferent pupillary deficit. Anterior segment examination and dilated fundoscopy were normal; no ocular movements were elicited when a large plain mirror was held in front of her. The rest of the neurological examination was normal. Serum magnesium was reduced to 0.1 mmol/l (reference range 0.7–1.2 mmol/l). Electroencephalography showed diffuse slowing confirming an encephalopathy.

• An 84-year-old woman with adenocarcinoma of the ovary had two fully reversible episodes of non-convulsive encephalopathy, each following a course of cisplatin-based chemotherapy, confirming a causal relation [ ]. She developed acute confusion, a partial left homonymous hemianopia and a left extinction hemiparesthesia 7 and 10 days after treatment. Brain MRI showed long-standing cerebral microvascular changes and an electroencephalogram showed right-sided parieto-occipital periodic lateralized epileptiform discharges over a generalized background slowing of activity.

In view of the similarity to posterior leukoencephalopathy, the second case suggests regional endovascular injury rather than direct cerebral toxicity as the initial event in the evolution of encephalopathy.

Strokes have been reported in patients receiving cisplatin.

• A 21-year-old woman with a mixed germ cell tumor of the left ovary was given intravenous chemotherapy including etoposide 100 mg/m ² on days 1–5, cisplatin 20 mg/m ² on days 1–5, and bleomycin 30 units on days 2, 8, and 15, all of which she tolerated very well [ ].Three weeks later she received a second cycle, which was complicated by an episode of dizziness on day 8. The following day she had an episode of transient dysphasia for 10 minutes. Her third course was uneventful until day 7, when she collapsed with a severe right-sided hemiparesis and dysphasia. Left-sided total anterior circulation infarction was confirmed on MRI scan.

• A 31-year-old man with a seminoma had an orchidectomy, followed by chemotherapy with cisplatin, etoposide, and bleomycin [ ]. A day after the end of the second course of chemotherapy he became comatose with a heart rate of 150/minute and a systolic blood pressure of 80 mmHg. Cranial angiography showed a thrombosis of the basilar artery and a cranial CT scan showed cerebellar infarction but no brain metastases.

However, the use of other drugs in these patients makes it difficult to assign causality to cisplatin.

Infusions of cisplatin into the axillary artery have led to a bronchial plexopathy rather than the more commonly described lumbosacral nerve plexus lesion [ ].

In five patients cerebral herniation followed cisplatin therapy [ ]. However, all had evidence of an intra-cerebral tumor with mass effect and the herniation of the brain was thought to be multifactorial rather than directly attributable to cisplatin.

Auditory brainstem responses have been used to detect ototoxicity from cisplatin and carboplatin when used in combination therapy [ ].

Mechanism and susceptibility factors

The mechanism of cisplatin-induced neurotoxicity has not been fully explained. Cisplatin appears to affect neurons in the dorsal root ganglia. It has also been suggested that it can act as a calcium channel blocker, altering intra-cellular calcium homeostasis and leading to apoptosis of exposed neurons, such as those of the dorsal root ganglia. Cisplatin-induced sensory neuropathy is predominantly characterized by symptoms such as numbness and tingling, paresthesia of the upper and lower extremities, reduced deep-tendon reflexes, and leg weakness with gait disturbance. The first symptoms are often observed after a cumulative dose of 300–600 mg/m ² . Risk factors include diabetes mellitus, alcohol consumption, or inherited neuropathies. Advanced age has not been identified as an independent susceptibility factor when there is no co-morbidity [ ].

The acute neurotoxic effects of oxaliplatin may result from drug-related inhibition of voltage-gated sodium currents [ ]. It has been suggested that oxalate ions, which are released during oxaliplatin metabolism, might be responsible for the inhibitory effects on the voltage-gated sodium channels, because of their calcium-chelating activity. Whether there are calcium-sensitive, voltage-gated sodium channels that can be affected by oxalate-induced calcium depletion or whether an indirect effect through changes in intracellular calcium-dependent regulatory mechanisms contributes to oxaliplatin-induced sensory neuropathy needs further investigation [ ].

The risk of oxaliplatin-induced neurosensory toxicity may be increased after surgery. Of 12 patients with meta-static colorectal cancer, seven reported immediate postoperative aggravation of pre-existing neurotoxicity. Before surgery, they had only acral paresthesia without any functional impairment, whereas after surgery they complained of major worsening of symptoms, including loss of hand grip strength, leading to dependence in dressing, eating, and use of the toilet, or loss of sensitivity, interfering with walking, which could persist for several months [ ]. The authors speculated that perioperative hemolysis had caused an increase in unconjugated bilirubin and the release of ultrafilterable oxaliplatin, which had previously been confined to the intraerythrocytic compartment. In addition, diffusion of ultrafilterable oxaliplatin out of erythrocytes into the plasma during hemodilution can contribute to the undesirable perioperative increase in unbound oxaliplatin in the plasma.

There is a correlation between the total dose of cisplatin and the vibratory perception threshold of the hand [ ].

Dose-relatedness

When three different schedules of cisplatin were evaluated with regard to the drug’s neurotoxicity, using the same dose of 450 mg/m ² for each of the schedules, it was found that cisplatin-induced peripheral neuropathy depended on both total-dose and single-dose intensity [ ].

Neurotoxicity in 22 adolescents was related to the prior cumulative dose of cisplatin that had been received; the relative risk increased 3.2-fold up to a dose of 600 mg/m ² , and 4.1-fold up to a dose of 1340 mg/m ² [ ].

By comparing 50 mg/m ² weekly with 75 mg/m ² three times weekly, using detailed neurological and neurophysiological examination, it has been concluded that cisplatin neuropathy is either of sensory or axonal type, and that both are related to total and single doses [ ]. However, others have suggested that cisplatin-induced peripheral neurotoxicity is related to dose intensity rather than to the total dose received [ ].

A 4-year follow-up of comparison of a combination of cyclophosphamide with cisplatin either 50 or 100 mg/m ² in ovarian cancer has been reported [ ]. Peripheral neuropathy was dose-limiting and persistent. Ten of 31 patients had significant toxicity in the high-dose group compared with one of 24 in the low-dose group.

High-dose cisplatin therapy . The use of aggressive hydration using hypertonic saline and sodium thiosulfate, with dose-scheduling, reduces the risks of dose-limiting nephrotoxicity of cisplatin, and this has made possible the use of high-dose cisplatin (over 200 mg/m ² per course). However, such doses can cause severe chronic peripheral neuropathy, ototoxicity, and myelosuppression, although these effects can be reduced by lengthening the infusion time of cisplatin [ ]. Peripheral neuropathy is the commonest manifestation of cisplatin neurotoxicity; with high-dose administration the incidence and severity increase with the total dose, and it appears to be age-related. It was not seen in 47 children treated with high-dose cisplatin (40 mg/m ² /day for 5 days) for neuroblastoma [ ]. Autonomic neuropathy, motor neuropathy, and denervation changes in muscles occur occasionally.

In a clinical and electrophysiological study of eight patients treated with high-dose cisplatin (800–1400 mg) plus etoposide and bleomycin, all developed a peripheral sensory neuropathy [ ]. A reduction in vibratory sensation was the earliest manifestation of the neuropathy and the findings were compatible with primary damage to the dorsal root ganglia with a central-distal axonopathy. No motor nerve abnormalities were detected, apart from one patient with carpal tunnel syndrome, but two patients had prolonged brain-stem auditory-evoked potentials, indicating a central transmission defect. In another clinical and electrophysiological study of seven patients treated with cisplatin, the sensory neuropathy was also axonal, with considerable involvement of proprioception [ ]. Postmortem study in one case showed degeneration of the posterior columns of the spinal cord and evidence of neuronal loss in the lumbar spinal ganglion.

Eleven patients referred for neurological evaluation after cisplatin infusion into the internal or external iliac arteries for pelvic or lower limb tumors all developed symptoms within 48 hours of nerve or plexus dysfunction within the territory supplied by the cannulated artery [ ]. The lumbosacral plexus was affected in nine patients, the femoral nerve in one, and the peroneal nerve in one. The doses of cisplatin ranged from 50 to 160 mg/m ² and they did not correlate with the severity or course of the neuropathy. Small-vessel injury and infarction or a direct toxic effect are likely explanations.

Time-course

In a study of the time-course and prognosis of cisplatin-induced neurotoxicity (for example sural nerve sensory action, conduction velocity, and vibration threshold in the left big toe) in 29 patients with metastatic germ cell tumors, the onset of paresthesia was delayed [ ]. After completion of chemotherapy (3–4 cycles) only 11% of the patients had neurotoxic symptoms, whereas 3 months later the proportion was 65%. Cisplatin-induced neurological disorders should therefore be evaluated at 1–4 months after the end of weekly cisplatin administration, because during this time the most severe form of cisplatin neurotoxicity is to be expected. There was resolution of symptoms in most of the patients over the next 12 months, suggesting that in some individuals a long period of regeneration is required to restore axonal sensory function. In patients with mild signs of cisplatin-related neuropathy, retreatment is generally feasible after several months [ , ].

Management

Among several thiol compounds, glutathione may provide neuroprotection in patients treated with cisplatin without altering its antineoplastic activity. This protective role may be based on blockade of the accumulation of p53 protein in response to platinum in dorsal root ganglia, thereby hindering platinum-based apoptosis [ , ].

The melanocortin Org2766, an ACTH analogue, which is not yet available for clinical use, alleviates neurotoxicity due to vinca alkaloids and cisplatin, perhaps by enhancing neural repair. However, whereas preliminary results suggested some neuroprotection in women with ovarian cancer treated with cisplatin, these results were not confirmed in a randomized, multicenter, double-blind, placebo-controlled dose-finding study, even with higher doses of Org 2766 [ ].

There is evidence that amifostine can reduce the frequency of cisplatin-induced peripheral neuropathy, allowing higher mean cumulative doses to be used. However, some of the results should be interpreted with caution, because the studies included patients who differed in respect to treatment regimen, disease states, and pretreatment status. The underlying protective effect of amifostine may be based on its capacity to scavenge free radicals and prevent cisplatin DNA adduct formation in several organs, including the dorsal root ganglia [ ]. In a pilot study in 15 patients, subcutaneous amifostine was given 20 minutes before oxaliplatin, in order to counteract oxaliplatin-induced peripheral neurosensory toxicity. In 10 patients, this regimen reduced the severity of cumulative neuropathy without compromising antitumor efficacy; the amifostine was well tolerated [ ].

There is increasing evidence that acute oxaliplatin-induced neurotoxicity can be improved by intravenous infusion of calcium gluconate 1000 mg and magnesium sulfate heptahydrate 1000 mg before and after oxaliplatin. It has recently been shown that this strategy could reduce the incidence of acute neurotoxic symptoms, including laryngopharyngeal dysesthesia. Of 101 patients with advanced colorectal cancers who received folinic acid (leucovorin), 5-fluorouracil, and oxaliplatin (85 mg/m ² every 2 weeks, 20 patients; 100 mg/m ² every 2 weeks, 22 patients; 130 mg/m ² every 3 weeks, 59 patients), 63 received infusions of calcium and magnesium (1 g each) before and after oxaliplatin administration (treatment group); 38 patients (control group) did not receive infusions of calcium + magnesium. The median cumulative dose of oxaliplatin was 910 (range 255–2340) mg/m ² in the calcium/magnesium group and 650 (range 255–1450) mg/m ² in the control group. At the end of treatment, 27% had neuropathy (any grade) compared with 75% in the control group; 1.6% and 26% had pharyngolaryngeal dysesthesia; and 5% and 24% had grade 3 neuropathy. However, further studies are warranted before this regimen can be generally recommended for reducing the risk of acute neurosensory symptoms associated with oxaliplatin infusion [ , ].

Carbamazepine is a potent sodium channel blocker and has therefore been studied in the prevention of oxaliplatin-induced neuropathy [ ]. The doses of carbamazepine were adjusted to produce serum concentrations in the range 30–60 mg/ml. None of the patients who took carbamazepine reported symptoms of peripheral neurotoxicity; however, two patients (one who forgot to take carbamazepine and one who stopped taking it because he felt tired) developed grade 1 peripheral sensory neurotoxicity. These symptoms were abolished when carbamazepine was restarted. One can therefore speculate that the concomitant use of carbamazepine may allow the use of a higher cumulative dose of oxaliplatin without the occurrence of grade-4 neuropathy. However, a multicenter trial is warranted to confirm these encouraging preliminary results [ ].

In 15 patients with metastatic colorectal cancer who were given gabapentin (100 mg bd or tds) if neuropathic symptoms developed with oxaliplatin, the symptoms disappeared in all patients, even in those who received up to 14 courses of oxaliplatin. Withdrawal of gabapentin resulted in recurrence. However, a controlled trial is required to verify these encouraging preliminary results.

It has been suggested that chronomodulated delivery of oxaliplatin might reduce the incidence of platinum-induced neurotoxicity [ , ]. In a randomized, multicenter trial in patients with previously untreated metastases from colorectal cancer, 93 patients were assigned chronotherapy and 93 were assigned constant-rate infusion [ ]. Chronotherapy reduced the rate of severe mucositis five-fold and halved the rate of functional impairment from peripheral sensitive neuropathy. Median and 3-year survival times were similar in the two groups.

Preliminary results have suggested that glutathione may be neuroprotective in patients receiving oxaliplatin [ ].