ZANOSAR

Zanosar should only be administered under the supervision of a physician experienced in the use of anti-cancer chemotherapeutic agents. The patient should have access to a facility with a laboratory and supportive resources sufficient to monitor drug tolerance and to protect and maintain a patient compromised by drug toxicity.

Posology The dose is based on the body surface area (m2).

Two different dosage schedules can be used:

Six-weekly regimen - 500 mg/m2/day, intravenously for 5 consecutive days every 6 weeks until maximum benefit is obtained or until treatment-limiting toxicity is observed. Dose escalation on this schedule is not recommended. Three-weekly regimen – 500 mg/m2/day, intravenously for 5 consecutive days during cycle 1, followed by 1000 mg/m2 every 3rd week during the subsequent cycles.

Other dosing regimens, with similar dose intensity, have been used in clinical studies with comparable efficacy and safety results. However, a single dose of 1500 mg/m2 of body surface area should not be exceeded (renal toxicity). The optimal duration of maintenance therapy with Zanosar has not been established.

For patients with functional tumours, serial monitoring of biological markers allows a determination of biochemical response to therapy. For patients with either functional or nonfunctional tumours, response to therapy can be determined by measurable reductions of tumour size on imaging.

4). Dose adjustment or discontinuation of the drug may be indicated, depending upon the degree of toxicity noted. Antiemetic premedication is recommended to prevent nausea and vomiting. 6). The duration of infusion should be between 30 minutes and 4 hours.

4). This medicinal product is vesicant in nature and as such should be administered with caution through a free-flowing line. In the event of extravasation, the administration should be discontinued immediately.

Special populations:

Patients with renal impairment: Based on clinical practice, the dose of Zanosar should be adapted according to renal function: dose reduction or treatment discontinuation is mandatory in the presence of significant renal toxicity. 4) If GFR is comprised between 30 and 45 ml/min, the benefit/risk ratio should be thoroughly evaluated in a multidisciplinary approach, which includes soliciting a nephrologist’s opinion and balancing the potential benefit against the known risk of serious renal damage.

The most common adverse reactions reported with Zanosar are gastrointestinal and renal disorders. The former are not life threatening but can be disturbing for the patient and may result in treatment discontinuation if very severe; the latter are indolent but potentially serious.

The frequency and intensity of nausea and vomiting has decreased over time, due to the utilization of efficacious antiemetic drugs. Renal toxicity can be avoided or reduced with careful assessment of renal function before and during treatment, patient hydration during streptozocin administration, and dose adjustment in case of renal function impairment.

Streptozocin has the potential to cause hyperglycaemia due to its mechanism of action; however, glucose intolerance or diabetes have been rarely reported in clinical practice. Myelotoxicity is usually mild and transient. Hepatic toxicity has been described, but not reported as a major issue during treatment.

Tabulated list of adverse reactions (from published data and post-marketing experience): Adverse reactions are listed below by MedDRA system organ class and frequency using the following convention: very common (≥1/10), common (≥ 1/100 to < 1/10), uncommon (≥1/1,000 to < 1/100) and not known (cannot be estimated from the available data).

MedDRA system organ class Very common adverse reactions Common adverse reactions Frequency not known Blood and lymphatic system disorders Decreased haematocrit, leukocytes and platelet counts Metabolism and nutrition disorders glucose intolerance Nervous system disorders Confusion, lethargy, depression Gastrointestinal
disorders Severe nausea and vomiting, Diarrhoea Nephrogenic diabetes insipidus Hepatobiliary disorders Elevated liver enzymes (SGOT and LDH) Hepatotoxicity Hypoalbuminemia Renal and urinary disorders Renal toxicity – proteinuria, proximal tubular injury, phosphaturia, acute renal failure Urinary disorders General disorders and administration site conditions Fever, Injection site reactions Gastrointestinal disorders: Patients treated with Zanosar have experienced nausea and vomiting.

Renal Toxicity
:

Many patients treated with Zanosar have experienced some degree of renal toxicity, as evidenced by an increase in plasma creatinine and proteinuria. The mechanisms of renal toxicity are still unclear but experimental and clinical data suggest tubular toxicity, such as tubular acidosis, low molecular weight proteinuria, hypokalemia and hypocalcaemia.

Such toxicity is dose-related and cumulative in most cases and may be severe or fatal. However, it can also appear after the first administration. Renal function must be monitored immediately before and two weeks after each course of therapy.

Routine surveillance consists of the measurement of plasma creatinine with the evaluation of glomerular filtration rate (GFR) by the Modification of Diet in Renal Diseases (MDRD) formula. e. before the first cycle of therapy) and two to four weeks after the end of the last cycle of therapy, proteinuria and serum electrolytes should also be measured, in addition to plasma creatinine.

2). 9% before the administration of Zanosar may help reduce the risk of toxicity to the renal tubular epithelium by decreasing renal and urinary concentration of the drug and its metabolites. Use of Zanosar in patients with preexisting renal disease requires a judgment by the physician of the potential benefit of treatment as opposed to the known risk of serious renal damage.

This drug should not be used concomitantly with other potential nephrotoxic drugs.

Hepatotoxicity:

Liver function tests should be done on a regular basis, to detect hepatic toxicity. Reduction of the dose or discontinuation should be considered in case of hepatic toxicity.

Haematologic toxicity:

Complete blood counts should be done on a regular basis, to detect haematologic toxicity. Reduction of the dose or discontinuation should be considered in case of haematologic toxicity (usually due to the association of Zanosar with another chemotherapy).

4) • Live and live-attenuated vaccines • Breastfeeding