• Treatment of invasive candidiasis in adult or paediatric patients.
• Treatment of invasive aspergillosis in adult or paediatric patients who are refractory to
or intolerant of amphotericin B, lipid formulations of amphotericin B and/or
itraconazole. Refractoriness is defined as progression of infection or failure to improve
after a minimum of 7 days of prior therapeutic doses of effective antifungal therapy.
• Empirical therapy for presumed fungal infections (such as Candida or Aspergillus) in
febrile, neutropaenic adult or paediatric patients.

Caspofungin should be initiated by a physician experienced in the management of invasive
fungal infections.
Posology
Adult patients
A single 70 mg loading dose should be administered on Day-1, followed by 50 mg daily
thereafter. In patients weighing more than 80 kg, after the initial 70 mg loading dose,

caspofungin 70 mg daily is recommended (see section 5.2). No dosage adjustment is necessary
based on gender or race (see section 5.2).
Paediatric patients (12 months to 17 years)
In paediatric patients (12 months to 17 years of age), dosing should be based on the patient's
body surface area (see Instructions for Use in Paediatric Patients, Mosteller1 Formula). For all
indications, a single 70-mg/m2 loading dose (not to exceed an actual dose of 70 mg) should be
administered on Day 1, followed by 50 mg/m2 daily thereafter (not to exceed an actual dose of
70 mg daily). If the 50-mg/m2 daily dose is well tolerated but does not provide an adequate
clinical response, the daily dose can be increased to 70 mg/m2 daily (not to exceed an actual
daily dose of 70 mg).
The safety and efficacy of caspofungin have not been sufficiently studied in clinical trials
involving neonates and infants below 12 months of age. Caution is advised when treating this
age group. Limited data suggest that caspofungin at 25 mg/m2 daily in neonates and infants
(less than 3 months of age) and 50 mg/m2 daily in young children (3 to 11 months of age) can
be considered (see section 5.2).
Duration of treatment
Duration of empirical therapy should be based on the patient's clinical response. Therapy
should be continued until up to 72 hours after resolution of neutropaenia (ANC≥ 500). Patients
found to have a fungal infection should be treated for a minimum of 14 days and treatment
should continue for at least 7 days after both neutropaenia and clinical symptoms are resolved.
Duration of treatment of invasive candidiasis should be based upon the patient's clinical and
microbiological response. After signs and symptoms of invasive candidiasis have improved
and cultures have become negative, a switch to oral antifungal therapy may be considered. In
general, antifungal therapy should continue for at least 14 days after the last positive culture.
Duration of treatment of invasive aspergillosis is determined on a case by case basis and should
be based upon the severity of the patient's underlying disease, recovery from
immunosuppression, and clinical response. In general, treatment should continue for at least 7
days after resolution of symptoms.
The safety information on treatment durations longer than 4 weeks is limited. However,
available data suggest that caspofungin continues to be well tolerated with longer courses of
therapy (up to 162 days in adult patients and up to 87 days in paediatric patients).
Special populations
Elderly patients
In elderly patients (65 years of age or more), the area under the curve (AUC) is increased by
approximately 30 %. However, no systematic dosage adjustment is required. There is limited
treatment experience in patients 65 years of age and older (see section 5.2).

Renal impairment
No dosage adjustment is necessary based on renal impairment (see section 5.2).
Hepatic impairment
For adult patients with mild hepatic impairment (Child-Pugh score 5 to 6), no dosage
adjustment is needed. For adult patients with moderate hepatic impairment (Child-Pugh score 7
to 9), caspofungin 35 mg daily is recommended based upon pharmacokinetic data. An initial 70
mg loading dose should be administered on Day-1. There is no clinical experience in adult
patients with severe hepatic impairment (Child-Pugh score greater than 9) and in paediatric
patients with any degree of hepatic impairment (see section 4.4).
Co-administration with inducers of metabolic enzymes
Limited data suggest that an increase in the daily dose of caspofungin to 70 mg, following the
70 mg loading dose, should be considered when co-administering caspofungin in adult patients
with certain inducers of metabolic enzymes (see section 4.5). When caspofungin is coadministered
to paediatric patients (12 months to 17 years of age) with these same inducers of
metabolic enzymes (see section 4.5), a caspofungin dose of 70-mg/m2 daily (not to exceed an
actual daily dose of 70 mg) should be considered.
Method of administration
After reconstitution and dilution, the solution should be administered by slow intravenous
infusion over approximately 1 hour. For reconstitution directions see section 6.6.
Both 70 mg and 50 mg vials are available.
Caspofungin should be given as a single daily infusion.

Hypersensitivity to the active substance or to any of the excipients listed in section 6.1.

Anaphylaxis has been reported during administration of caspofungin. If this occurs,
caspofungin should be discontinued and appropriate treatment administered. Possibly
histamine-mediated adverse reactions, including rash, facial swelling, angioedema, pruritus,
sensation of warmth, or bronchospasm have been reported and may require discontinuation
and/or administration of appropriate treatment.
Limited data suggest that less common non-Candida yeasts and non-Aspergillusmoulds are not
covered by caspofungin. The efficacy of caspofungin against these fungal pathogens has not
been established.
Concomitant use of caspofungin with ciclosporin has been evaluated in healthy adult
volunteers and in adult patients. Some healthy adult volunteers who received two 3 mg/kg
doses of ciclosporin with caspofungin showed transient increases in alanine transaminase

(ALT) and aspartate transaminase (AST) of less than or equal to 3-fold the upper limit of
normal (ULN) that resolved with discontinuation of the treatment. In a retrospective study of
40 patients treated during marketed use with caspofungin and ciclosporin for 1 to 290 days
(median 17.5 days), no serious hepatic adverse reactions were noted. These data suggest that
casopofungin can be used in patients receiving ciclosporin when the potential benefit
outweighs the potential risk. Close monitoring of liver enzymes should be considered if
caspofungin and ciclosporin are used concomitantly.
In adult patients with mild and moderate hepatic impairment, the AUC is increased about 20%
and 75 %, respectively. A reduction of the daily dose to 35 mg is recommended for adults with
moderate hepatic impairment. There is no clinical experience in adults with severe hepatic
impairment or in paediatric patients with any degree of hepatic impairment. A higher exposure
than in moderate hepatic impairment is expected and caspofungin should be used with caution
in these patients (see sections 4.2 and 5.2).
Laboratory abnormalities in liver function tests have been seen in healthy volunteers and adult
and paediatric patients treated with caspofungin. In some adult and paediatric patients with
serious underlying conditions who were receiving multiple concomitant medications with
caspofungin, cases of clinically significant hepatic dysfunction, hepatitis and hepatic failure
have been reported; a causal relationship to caspofungin has not been established. Patients who
develop abnormal liver function tests during caspofungin therapy should be monitored for
evidence of worsening hepatic function and the risk/benefit of continuing caspofungin therapy
should be re-evaluated.
This medicinal product contains sucrose. Patients with rare hereditary problems of fructose
intolerance or sucrase-isomaltase insufficiency should not take this medicinal product (see
section 2).
Cases of Stevens-Johnson Syndrome (SJS) and toxic epidermal necrolysis (TEN) have been
reported after post-marketing use of caspofungin. Caution should apply in patients with history
of allergic skin reaction

Studies in vitro show that caspofungin is not an inhibitor of any enzyme in the cytochrome
P450 (CYP) system. In clinical studies, caspofungin did not induce the CYP3A4 metabolism of
other substances. Caspofungin is not a substrate for P-glycoprotein and is a poor substrate for
cytochrome P450 enzymes. However, caspofungin has been shown to interact with other
medicinal products in pharmacological and clinical studies (see below).
In two clinical studies performed in healthy adult subjects, ciclosporin A (one 4 mg/kg dose or
two 3 mg/kg doses 12 hours apart) increased the AUC of caspofungin by approximately 35 %.
These AUC increases are probably due to reduced uptake of caspofungin by the liver.
Caspofungin did not increase the plasma levels of ciclosporin. There were transient increases in
liver ALT and AST of less than or equal to 3-fold the upper limit of normal (ULN) when
caspofungin and ciclosporin were co-administered, that resolved with discontinuation of the
medicinal products. In a retrospective study of 40 patients treated during marketed use with

caspofungin and ciclosporin for 1 to 290 days (median 17.5 days), no serious hepatic adverse
reactions were noted (see section 4.4). Close monitoring of liver enzymes should be considered
if the two medicinal products are used concomitantly.
Caspofungin reduced the trough concentration of tacrolimus by 26 % in healthy adult
volunteers. For patients receiving both therapies, standard monitoring of tacrolimus blood
concentrations and appropriate tacrolimus dosage adjustments are mandatory.
Clinical studies in healthy adult volunteers show that the pharmacokinetics of caspofungin are
not altered to a clinically relevant extent by itraconazole, amphotericin B, mycophenolate,
nelfinavir, or tacrolimus. Caspofungin did not influence the pharmacokinetics of amphotericin
B, itraconazole, rifampicin or mycophenolatemofetil. Although safety data are limited it
appears that no special precautions are needed when amphotericin B, itraconazole, nelfinavir or
mycophenolatemofetil are co-administered with caspofungin.
Rifampicin caused a 60 % increase in AUC and 170 % increase in trough concentration of
caspofungin on the first day of co-administration when both medicinal products were initiated
together in healthy adult volunteers. Caspofungin trough levels gradually decreased upon
repeated administration. After two weeks' administration rifampicin had limited effect on
AUC, but trough levels were 30 % lower than in adult subjects who received caspofungin
alone. The mechanism of interaction could possibly be due to an initial inhibition and
subsequent induction of transport proteins. A similar effect could be expected for other
medicinal products that induce metabolic enzymes. Limited data from population
pharmacokinetics studies indicate that concomitant use of caspofungin with the inducers
efavirenz, nevirapine, rifampicin, dexamethasone, phenytoin, or carbamazepine may result in a
decrease in caspofungin AUC. When co-administering inducers of metabolic enzymes, an
increase in the daily dose of caspofungin to 70 mg, following the 70 mg loading dose, should
be considered in adult patients (see section 4.2).
All adult drug-drug interaction studies described above were conducted at a 50 or 70 mg daily
caspofungin dose. The interaction of higher doses of caspofungin with other medicinal
products has not been formally studied.
In paediatric patients, results from regression analyses of pharmacokinetic data suggest that coadministration
of dexamethasone with caspofungin may result in clinically meaningful
reductions in caspofungin trough concentrations. This finding may indicate that paediatric
patients will have similar reductions with inducers as seen in adults. When caspofungin is coadministered
to paediatric patients (12 months to 17 years of age) with inducers of drug
clearance, such as rifampicin, efavirenz, nevirapine, phenytoin, dexamethasone, or
carbamazepine, a caspofungin dose of 70-mg/m2 daily (not to exceed an actual daily dose of 70
mg) should be considered.

 

Pregnancy
There are no or limited data from the use of caspofungin in pregnant women. Caspofungin
should not be used during pregnancy unless clearly necessary. Animal studies have shown
developmental toxicity (see section 5.3). Caspofungin has been shown to cross the placental
barrier in animal studies.
Breastfeeding
It is unknown whether caspofungin is excreted in human milk. Available pharmacodynamic/
toxicological data in animals have shown excretion of caspofungin in milk. Women receiving
caspofungin should not breast-feed.
Fertility
For caspofungin, there were no effects on fertility in studies conducted in male and female rats
(see section 5.3). There are no clinical data for caspofungin to assess its impact on fertility.

No studies on the effects on the ability to drive and use machines have been performed.

Hypersensitivity reactions (anaphylaxis and possibly histamine-mediated adverse reactions)
have been reported (see section 4.4).
Also reported in patients with invasive aspergillosis were pulmonary oedema, adult respiratory
distress syndrome (ARDS), and radiographic infiltrates.
Adult Patients
In clinical studies, 1,865 adult individuals received single or multiple doses of caspofungin:
564 febrile neutropaenic patients (empirical therapy study), 382 patients with invasive
candidiasis, 228 patients with invasive aspergillosis, 297 patients with localisedCandida
infections, and 394 individuals enrolled in Phase I studies. In the empirical therapy study
patients had received chemotherapy for malignancy or had undergone haematopoietic stem-cell
transplantation (including 39 allogeneic transplantations). In the studies involving patients with
documented Candida infections, the majority of the patients with invasive Candida infections
had serious underlying medical conditions (e.g., haematologic or other malignancy, recent
major surgery, HIV) requiring multiple concomitant medications. Patients in the noncomparative
Aspergillus study often had serious predisposing medical conditions (e.g., bone
marrow or peripheral stem cell transplants, haematologic malignancy, solid tumours or organ
transplants) requiring multiple concomitant medications.
Phlebitis was a commonly reported local injection-site adverse reaction in all patient
populations. Other local reactions included erythema, pain/tenderness, itching, discharge, and a
burning sensation.
Reported clinical and laboratory abnormalities among all adults treated with caspofungin (total
1,780) were typically mild and rarely led to discontinuation.

The following adverse reactions were reported:
[Very common (≥ 1/10), Common (≥ 1/100 to < 1/10), Uncommon (≥1/1,000 to <1/100)]
Blood and lymphatic system disorders:
Common:haemoglobin decreased, haematocrit decreased, white blood cell count decreased
Uncommon:anaemia, thrombocytopaenia, coagulopathy, leukopaenia, eosinophil count
increased, platelet count decreased, platelet count increased, lymphocyte count decreased,
white blood cell count increased, neutrophil count decreased
Metabolism and nutrition disorders:
Common: hypokalemia
Uncommon: fluid overload, hypomagnesaemia, anorexia, electrolyte imbalance,
hyperglycaemia, hypocalcaemia, metabolic acidosis
Psychiatric disorders
Uncommon: anxiety, disorientation, insomnia
Nervous system disorders:
Common: headache
Uncommon: dizziness, dysgeusia, paraesthesia, somnolence, tremor, hypoaesthesia
Eye disorders:
Uncommon: ocular icterus, vision blurred, eyelid oedema, lacrimation increased
Cardiac disorders:
Uncommon: palpitations, tachycardia, arrhythmia, atrial fibrillation, cardiac failure congestive
Vascular disorders:
Common: phlebitis
Uncommon: thrombophlebitis, flushing, hot flush, hypertension, hypotension
Respiratory, thoracic and mediastinal disorders:
Common:dyspnoea
Uncommon: nasal congestion, pharyngolaryngeal pain, tachypnoea, bronchospasm, cough,
dyspnoea paroxysmal nocturnal, hypoxia, rales, wheezing
Gastrointestinal disorders:
Common: nausea, diarrhoea, vomiting
Uncommon: abdominal pain, abdominal pain upper, dry mouth, dyspepsia, stomach
discomfort, abdominal distension, ascites, constipation, dysphagia, flatulence
Hepatobiliary disorders:
Common: elevated liver values (alanine aminotransferase, aspartate aminotranserase, blood
alkaline phosphatase, bilirubin conjugated, blood bilirubin)

Unommon: cholestasis, hepatomegaly, hyperbilirubinaemia, jaundice, hepatic function
abnormal, hepatotoxicity, liver disorder, gamma-glutamyltransferase increased
Skin and subcutaneous tissue disorders:
Common: rash, pruritus, erythema, hyperhidrosis
Uncommon: erythema multiforme, rash macular, rash maculo-papular, rash pruritic, urticaria,
dermatitis allergic, pruritus generalised, rash erythematous, rash generalised, rash morbilliform,
skin lesion
Not known (cannot be estimated from available data): Toxic epidermal necrolysis and Stevens-
Johnson syndrome
Musculoskeletal and connective tissue disorders
Common: arthralgia
Uncommon: back pain, pain in extremity, bone pain, muscular weakness, myalgia
Renal and urinary disorders
Uncommon: renal failure, renal failure acute
General disorders and administration site conditions:
Common: pyrexia, chills, infusion-site pruritus
Uncommon: pain, catheter site pain, fatigue, feeling cold, feeling hot, infusion site erythema,
infusion site induration, infusion site pain, infusion site swelling, injection site phlebitis,
oedema peripheral, tenderness, chest discomfort, chest pain, face oedema, feeling of body
temperature change, induration, infusion site extravasation, infusion site irritation, infusion site
phlebitis, infusion site rash, infusion site urticaria, injection site erythema, injection site
oedema, injection site pain, injection site swelling, malaise, oedema
Investigations:
Common: blood potassium decreased, blood albumin decreased
Uncommon: blood creatinine increased, red blood cells urine positive, protein total decreased,
protein urine present, prothrombin time prolonged, prothrombin time shortened, blood sodium
decreased, blood sodium increased, blood calcium decreased, blood calcium increased, blood
chloride decreased, blood glucose increased, blood magnesium decreased, blood phosphorus
decreased, blood phosphorus increased, blood urea increased, activated partial thromboplastin
time prolonged, blood bicarbonate decreased, blood chloride increased, blood potassium
increased, blood pressure increased, blood uric acid decreased, blood urine present, breath
sounds abnormal, carbon dioxide decreased, immunosuppressant drug level increased,
international normalised ratio increased, urinary casts, white blood cells urine positive, and pH
urine increased.
Caspofungin has also been evaluated at 150 mg daily (for up to 51 days) in 100 adult patients
(see section 5.1). The study compared caspofungin at 50 mg daily (following a 70-mg loading
dose on Day 1) versus 150 mg daily in the treatment of invasive candidiasis. In this group of
patients, the safety of caspofungin at this higher dose appeared generally similar to patients
receiving the 50-mg daily dose of caspofungin. The proportion of patients with a serious drug-

related adverse reaction or a drug-related adverse reaction leading to caspofungin
discontinuation was comparable in the 2 treatment groups.
Paediatric Patients
Data from 5 clinical studies completed in 171 paediatric patients suggest that the overall
incidence of clinical adverse experiences (26.3%; 95% CI -19.9, 33.6) is not worse than
reported for adults treated with caspofungin (43.1%; 95% CI -40.0, 46.2). However, paediatric
patients probably have a different adverse event profile compared to adult patients. The most
common drug-related clinical adverse experiences reported in paediatric patients treated with
caspofungin were pyrexia (11.7%), rash (4.7%) and headache (2.9%).
The following adverse reactions were reported:
[Very common (≥ 1/10), Common (≥ 1/100 to <1/10)]
Blood and lymphatic system disorders:
Common: eosinophil count increased
Nervous system disorders:
Common: headache
Cardiac disorders:
Common: tachycardia
Vascular disorders:
Common: flushing, hypotension
Hepatobiliary disorders:
Common: elevated liver enzyme levels (AST, ALT)
Skin and subcutaneous tissue disorders:
Common: rash, pruritus
General disorders and administration site conditions:
Very common: fever
Common: chills, catheter site pain
Investigations:
Common: decreased potassium, hypomagnesaemia, increased glucose, decreased phosphorus,
and increased phosphorus
Post-Marketing experience:
The following post-marketing adverse reactions have been reported:
Hepatobiliary disorders:
Hepatic dysfunction, gamma-glutamyltransferase increased

General disorders and administration site conditions:
Swelling and peripheral oedema
Investigations:
Hypercalcaemia
Reporting of suspected adverse reactions
Reporting suspected adverse reactions after authorisation of the medicinal product is important.
It allows continued monitoring of the benefit/risk balance of the medicinal product.

 

	To report any side effect(s): - The National Pharmacovigilance and Drug Safety Centre (NPC) o Fax: +966-11-205-7662 o Call NPC at +966-11-2038222, Exts: 2317-2356-2353-2354-2334-2340. o Toll free phone: 8002490000 o E-mail: npc.drug@sfda.gov.sa o Website: www.sfda.gov.sa/npc

 

 

 

 

 

 

Inadvertent administration of up to 400 mg of caspofungin in one day has been reported. These
occurrences did not result in clinically important adverse reactions. Caspofungin is not
dialysable.

Pharmacotherapeutic group: antimycotics for systemic use, ATC Code: J02AX04

 

Mechanism of action

Caspofungin acetate is a semi-synthetic lipopeptide (echinocandin) compound synthesised from a fermentation product of Glarea lozoyensis. Caspofungin acetate inhibits the synthesis of beta (1,3)-D-glucan, an essential component of the cell wall of many filamentous fungi and yeast. Beta (1,3)-D-glucan is not present in mammalian cells.

Fungicidal activity with caspofungin has been demonstrated against Candida yeasts. Studies in vitro and in vivo demonstrate that exposure of Aspergillus to caspofungin results in lysis and death of hyphal apical tips and branch points where cell growth and division occur.

 

Pharmacodynamic effects

Caspofungin has in vitro activity against Aspergillus species (Aspergillus fumigatus [N = 75], Aspergillus flavus [N = 111], Aspergillus niger [N = 31], Aspergillus nidulans [N = 8], Aspergillus terreus [N = 52], and Aspergillus candidus [N = 3]). Caspofungin also has in vitro activity against Candida species (Candida albicans [N = 1,032], Candida dubliniensis [N = 100], Candida glabrata [N = 151], Candida guilliermondii [N = 67], Candida kefyr [N = 62], Candida krusei [N = 147], Candida lipolytica [N = 20], Candida lusitaniae [N = 80], Candida parapsilosis [N = 215], Candida rugosa [N = 1], and Candida tropicalis [N = 258]), including isolates with multiple resistance transport mutations and those with acquired or intrinsic resistance to fluconazole, amphotericin B, and 5-flucytosine. Susceptibility testing was performed according to a modification of both the Clinical and Laboratory Standards Institute (CLSI, formerly known as the National Committee for Clinical Laboratory Standards [NCCLS]) method M38-A2 (for Aspergillus species) and method M27-A3 (for Candida species). Standardised techniques for susceptibility testing have been established for yeasts by EUCAST. However, interpretive breakpoints for caspofungin have not been approved by EUCAST. Isolates of Candida with reduced susceptibility to caspofungin have been identified in a small number of patients during treatment (MICs for caspofungin >2 mg/L (4- to 30-fold MIC increases) have been reported using standardized MIC testing techniques approved by the CLSI).The mechanism of resistance identified was FKS1/FKS2 gene mutation. These cases have been associated with poor clinical outcomes. Development of in vitro resistance to caspofungin by Aspergillus species has been identified. In limited clinical experience, resistance to caspofungin in patients with invasive aspergillosis has been observed. The mechanism of resistance has not been established. The incidence of resistance to caspofungin by various clinical isolates of Candida and Aspergillus is rare.

 

Clinical efficacy and safety

Invasive Candidiasis in Adult Patients: Two hundred thirty-nine patients were enrolled in an initial study to compare caspofungin and amphotericin B for the treatment of invasive candidiasis. Twenty-four patients had neutropaenia. The most frequent diagnoses were bloodstream infections (candidaemia) (77 %, n=186) and Candida peritonitis (8 %, n=19); patients with Candida endocarditis, osteomyelitis, or meningitis were excluded from this study. Caspofungin 50 mg once daily was administered following a 70 mg loading dose, while amphotericin B was administered at 0.6 to 0.7 mg/kg/day to non-neutropaenic patients or 0.7 to 1.0 mg/kg/day to neutropaenic patients. The mean duration of intravenous therapy was 11.9 days, with a range of 1 to 28 days. A favourable response required both symptom resolution and microbiological clearance of the Candida infection. Two hundred twenty-four patients were included in the primary efficacy analysis (MITT analysis) of response at the end of IV study therapy; favourable response rates for the treatment of invasive candidiasis were comparable for caspofungin (73 % [80/109]) and amphotericin B (62 % [71/115]) [% difference 12.7 (95.6 % CI -0.7, 26.0)]. Among patients with candidaemia, favourable response rates at the end of IV study therapy were comparable for caspofungin (72 % [66/92]) and amphotericin B (63 % [59/94]) in the primary efficacy analysis (MITT analysis) [% difference 10.0 (95.0 % CI -4.5, 24.5)]. Data in patients with non-blood sites of infection were more limited. Favourable response rates in neutropaenic patients were 7/14 (50 %) in the caspofungin group and 4/10 (40 %) in the amphotericin B group. These limited data are supported by the outcome of the empirical therapy study.

 

In a second study, patients with invasive candidiasis received daily doses of caspofungin at 50 mg/day (following a 70-mg loading dose on Day 1) or caspofungin at 150 mg/day (see section 4.8). In this study, the caspofungin dose was administered over 2 hours (instead of the routine 1-hour administration). The study excluded patients with suspected Candida endocarditis, meningitis, or osteomyelitis. As this was a primary therapy study, patients who were refractory to prior antifungal agents were also excluded. The number of neutropenic patients enrolled in this study was also limited (8.0 %). Efficacy was a secondary endpoint in this study. Patients who met the entry criteria and received one or more doses of caspofungin study therapy were included in the efficacy analysis. The favorable overall response rates at the end of caspofungin therapy were similar in the 2 treatment groups: 72 % (73/102) and 78 % (74/95) for the caspofungin 50-mg and 150-mg treatment groups, respectively (difference 6.3 % [95 % CI -5.9, 18.4]).

 

Invasive Aspergillosis in Adult Patients: Sixty-nine adult patients (age 18-80) with invasive aspergillosis were enrolled in an open-label, non-comparative study to evaluate the safety, tolerability, and efficacy of caspofungin. Patients had to be either refractory to (disease progression or failure to improve with other antifungal therapies given for at least 7 days) (84 % of the enrolled patients) or intolerant of (16 % of enrolled patients) other standard antifungal therapies. Most patients had underlying conditions (haematologic malignancy [N = 24], allogeneic bone marrow transplant or stem cell transplant [N = 18], organ transplant [N = 8], solid tumour [N = 3], or other conditions [N = 10]). Stringent definitions, modelled after the Mycoses Study Group Criteria, were used for diagnosis of invasive aspergillosis and for response to therapy (favourable response required clinically significant improvement in radiographs as well as in signs and symptoms). The mean duration of therapy was 33.7 days, with a range of 1 to 162 days. An independent expert panel determined that 41 % (26/63) of patients receiving at least one dose of caspofungin had a favourable response. For those patients who received more than 7 days of therapy with caspofungin, 50 % (26/52) had a favourable response. The favourable response rates for patients who were either refractory to or intolerant of previous therapies were 36 % (19/53) and 70 % (7/10), respectively. Although the doses of prior antifungal therapies in 5 patients enrolled as refractory were lower than those often administered for invasive aspergillosis, the favourable response rate during therapy with caspofungin was similar in these patients to that seen in the remaining refractory patients (2/5 versus 17/48, respectively). The response rates among patients with pulmonary disease and extrapulmonary disease were 47 % (21/45) and 28 % (5/18), respectively. Among patients with extrapulmonary disease, 2 of 8 patients who also had definite, probable, or possible CNS involvement had a favourable response.

 

Empirical Therapy in Febrile, Neutropaenic Adult Patients: A total of 1,111 patients with persistent fever and neutropaenia were enrolled in a clinical study and treated with either caspofungin 50 mg once daily following a 70 mg loading dose or liposomal amphotericin B 3.0 mg/kg/day. Eligible patients had received chemotherapy for malignancy or had undergone hematopoietic stem-cell transplantation, and presented with neutropaenia (<500 cells/mm³ for 96 hours) and fever (>38.0°C) not responding to ≥ 96 hours of parenteral antibacterial therapy. Patients were to be treated until up to 72 hours after resolution of neutropaenia, with a maximum duration of 28 days. However, patients found to have a documented fungal infection could be treated longer. If the drug was well tolerated but the patient's fever persisted and clinical condition deteriorated after 5 days of therapy, the dosage of study drug could be increased to 70 mg/day of caspofungin (13.3 % of patients treated) or to 5.0 mg/kg/day of liposomal amphotericin B (14.3 % of patients treated). There were 1,095 patients included in the primary Modified Intention-To-Treat (MITT) efficacy analysis of overall favourable response; caspofungin (33.9 %) was as effective as liposomal amphotericin B (33.7 %) [% difference 0.2 (95.2 % CI –5.6, 6.0)]. An overall favourable response required meeting each of 5 criteria: (1) successful treatment of any baseline fungal infection (caspofungin 51.9 % [14/27], liposomal amphotericin B 25.9 % [7/27]), (2) no breakthrough fungal infections during administration of study drug or within 7 days after completion of treatment (caspofungin 94.8 % [527/556], liposomal amphotericin B 95.5 % [515/539]), (3) survival for 7 days after completion of study therapy (caspofungin 92.6 % [515/556], liposomal amphotericin B 89.2 % [481/539]), (4) no discontinuation from the study drug because of drug-related toxicity or lack of efficacy (caspofungin 89.7 % [499/556], liposomal amphotericin B 85.5 % [461/539]), and (5) resolution of fever during the period of neutropaenia (caspofungin 41.2 % [229/556], liposomal amphotericin B 41.4 % [223/539]). Response rates to caspofungin and liposomal amphotericin B for baseline infections caused by Aspergillus species were, respectively, 41.7 % (5/12) and 8.3 % (1/12), and by Candida species were 66.7 % (8/12) and 41.7 % (5/12). Patients in the caspofungin group experienced breakthrough infections due to the following uncommon yeasts and moulds: Trichosporon species (1), Fusarium species (1), Mucor species (1), and Rhizopus species (1).

 

Paediatric population

The safety and efficacy of caspofungin was evaluated in paediatric patients 3 months to 17 years of age in two prospective, multicenter clinical trials. The study design, diagnostic criteria, and criteria for efficacy assessment were similar to the corresponding studies in adult patients (see section 5.1).

 

The first study, which enrolled 82 patients between 2 to 17 years of age, was a randomized, double-blind study comparing caspofungin (50 mg/m² IV once daily following a 70-mg/m² loading dose on Day 1 [not to exceed 70 mg daily]) to liposomal amphotericin B (3 mg/kg IV daily) in a 2:1 treatment fashion (56 on caspofungin, 26 on liposomal amphotericin B) as empirical therapy in paediatric patients with persistent fever and neutropenia. The overall success rates in the MITT analysis results, adjusted by risk strata, were as follows: 46.6 % (26/56) for caspofungin and 32.2 % (8/25) for liposomal amphotericin B.

 

The second study was a prospective, open-label, non-comparative study estimating the safety and efficacy of caspofungin in paediatric patients (ages 6 months to 17 years) with invasive candidiasis, esophageal candidiasis, and invasive aspergillosis (as salvage therapy). Forty-nine patients were enrolled and received caspofungin at 50 mg/m² IV once daily following a 70-mg/m² loading dose on Day 1 (not to exceed 70 mg daily), of whom 48 were included in the MITT analysis. Of these, 37 had invasive candidiasis, 10 had invasive aspergillosis, and 1 patient had esophageal candidiasis. The favorable response rate, by indication, at the end of caspofungin therapy was as follows in the MITT analysis: 81 % (30/37) in invasive candidiasis, 50 % (5/10) in invasive aspergillosis, and 100 % (1/1) in esophageal candidiasis.

Distribution

Caspofungin is extensively bound to albumin. The unbound fraction of caspofungin in plasma varies from 3.5 % in healthy volunteers to 7.6 % in patients with invasive candidiasis. Distribution plays the prominent role in caspofungin plasma pharmacokinetics and is the rate-controlling step in both the alpha- and beta-disposition phases. The distribution into tissues peaked at 1.5 to 2 days after dosing when 92 % of the dose was distributed into tissues. It is likely that only a small fraction of the caspofungin taken up into tissues later returns to plasma as parent compound. Therefore, elimination occurs in the absence of a distribution equilibrium, and a true estimate of the volume of distribution of caspofungin is currently impossible to obtain.

 

Biotransformation

Caspofungin undergoes spontaneous degradation to an open ring compound. Further metabolism involves peptide hydrolysis and N-acetylation. Two intermediate products, formed during the degradation of caspofungin to this open ring compound, form covalent adducts to plasma proteins resulting in a low-level, irreversible binding to plasma proteins.

In vitro studies show that caspofungin is not an inhibitor of cytochrome P450 enzymes 1A2, 2A6, 2C9, 2C19, 2D6 or 3A4. In clinical studies, caspofungin did not induce or inhibit the CYP3A4 metabolism of other medicinal products. Caspofungin is not a substrate for P-glycoprotein and is a poor substrate for cytochrome P450 enzymes.

 

Elimination

The elimination of caspofungin from plasma is slow with a clearance of 10-12 ml/min. Plasma concentrations of caspofungin decline in a polyphasic manner following single 1-hour intravenous infusions. A short alpha-phase occurs immediately post-infusion, followed by a beta-phase with a half-life of 9 to 11 hours. An additional gamma-phase also occurs with a half-life of 45 hours. Distribution, rather than excretion or biotransformation, is the dominant mechanism influencing plasma clearance.

Approximately 75 % of a radioactive dose was recovered during 27 days: 41 % in urine and 34 % in faeces. There is little excretion or biotransformation of caspofungin during the first 30 hours after administration. Excretion is slow and the terminal half-life of radioactivity was 12 to 15 days. A small amount of caspofungin is excreted unchanged in urine (approximately 1.4 % of dose).

 

Caspofungin displays moderate non-linear pharmacokinetics with increased accumulation as the dose is increased, and a dose dependency in the time to reach steady state upon multiple-dose administration.

 

Special populations

Increased caspofungin exposure was seen in adult patients with renal impairment and mild liver impairment, in female subjects, and in the elderly. Generally the increase was modest and not large enough to warrant dosage adjustment. In adult patients with moderate liver impairment or in higher weight patients, a dosage adjustment may be necessary (see below).

Weight: Weight was found to influence caspofungin pharmacokinetics in the population pharmacokinetic analysis in adult candidiasis patients. The plasma concentrations decrease with increasing weight. The average exposure in an adult patient weighing 80 kg was predicted to be about 23 % lower than in an adult patient weighing 60 kg (see section 4.2).

Hepatic impairment: In adult patients with mild and moderate hepatic impairment, the AUC is increased about 20 and 75 %, respectively. There is no clinical experience in adult patients with severe hepatic impairment and in paediatric patients with any degree of hepatic impairment. In a multiple-dose study, a dose reduction of the daily dose to 35 mg in adult patients with moderate hepatic impairment has been shown to provide an AUC similar to that obtained in adult subjects with normal hepatic function receiving the standard regimen (see section 4.2).

 

Renal impairment: In a clinical study of single 70 mg doses, caspofungin pharmacokinetics were similar in adult volunteers with mild renal impairment (creatinine clearance 50 to 80 ml/min) and control subjects. Moderate (creatinine clearance 31 to 49 ml/min), advanced (creatinine clearance 5 to 30 ml/min), and end-stage (creatinine clearance <10 ml/min and dialysis dependent) renal impairment moderately increased caspofungin plasma concentrations after single-dose administration (range: 30 to 49 % for AUC). However, in adult patients with invasive candidiasis, oesophageal candidiasis, or invasive aspergillosis who received multiple daily doses of caspofungin 50 mg, there was no significant effect of mild to advanced renal impairment on caspofungin concentrations. No dosage adjustment is necessary for patients with renal impairment. Caspofungin is not dialysable, thus supplementary dosing is not required following haemodialysis.

Gender: Caspofungin plasma concentrations were on average 17-38 % higher in women than in men.

 

Elderly: A modest increase in AUC (28 %) and C_24h (32 %) was observed in elderly male subjects compared with young male subjects. In patients who were treated empirically or who had invasive candidiasis, a similar modest effect of age was seen in older patients relative to younger patients.

 

Race: Patient pharmacokinetic data indicated that no clinically significant differences in the pharmacokinetics of caspofungin were seen among Caucasians, Blacks, Hispanics, and Mestizos.

 

Paediatric Patients:

In adolescents (ages 12 to 17 years) receiving caspofungin at 50 mg/m² daily (maximum 70 mg daily), the caspofungin plasma AUC_0-24hr was generally comparable to that seen in adults receiving caspofungin at 50 mg daily. All adolescents received doses >50 mg daily, and, in fact, 6 of 8 received the maximum dose of 70 mg/day. The caspofungin plasma concentrations in these adolescents were reduced relative to adults receiving 70 mg daily, the dose most often administered to adolescents.

 

In children (ages 2 to 11 years) receiving caspofungin at 50 mg/m² daily (maximum 70 mg daily), the caspofungin plasma AUC_0-24hr after multiple doses was comparable to that seen in adults receiving caspofungin at 50 mg/day.

 

In young children and toddlers (ages 12 to 23 months) receiving caspofungin at 50 mg/m² daily (maximum 70 mg daily), the caspofungin plasma AUC_0-24hr after multiple doses was comparable to that seen in adults receiving caspofungin at 50 mg daily and to that in older children (2 to 11 years of age) receiving the 50 mg/m² daily dose.

 

Overall, the available pharmacokinetic, efficacy, and safety data are limited in patients 3 to 10 months of age. Pharmacokinetic data from one 10-month old child receiving the 50 mg/m² daily dose indicated an AUC_0-24hr within the same range as that observed in older children and adults at the 50 mg/m² and the 50 mg dose, respectively, while in one 6-month old child receiving the 50 mg/m² dose, the AUC_0-24hr was somewhat higher.

 

In neonates and infants (<3 months) receiving caspofungin at 25 mg/m² daily (corresponding mean daily dose of 2.1 mg/kg), caspofungin peak concentration (C_{1 hr}) and caspofungin trough concentration (C_{24 hr}) after multiple doses were comparable to that seen in adults receiving caspofungin at 50 mg daily. On Day 1, C_{1 hr} was comparable and C_{24 hr} modestly elevated (36 %) in these neonates and infants relative to adults. However, variability was seen in both C_{1 hr} (Day 4 geometric mean 11.73 µg/ml, range 2.63 to 22.05 µg/ml) and C_{24 hr} (Day 4 geometric mean 3.55 µg/ml, range 0.13 to 7.17 µg/ml). AUC_0-24hr measurements were not performed in this study due to the sparse plasma sampling. Of note, the efficacy and safety of caspofungin have not been adequately studied in prospective clinical trials involving neonates and infants under 3 months of age.

 

Repeated dose toxicity studies in rats and monkeys using doses up to 7-8 mg/kg given
intravenously showed injection site reactions in rats and monkeys, signs of histamine release in
rats, and evidence of adverse effects directed at the liver in monkeys. Developmental toxicity
studies in rats showed that caspofungin caused decreases in foetal body weights and an
increase in the incidence of incomplete ossification of vertebra, sternebra, and skull bone at
doses of 5 mg/kg that were coupled to adverse maternal effects such as signs of histamine
release in pregnant rats. An increase in the incidence of cervical ribs was also noted.
Caspofungin was negative in in vitro assays for potential genotoxicity as well as in the in vivo
mouse bone marrow chromosomal test. No long-term studies in animals have been performed
to evaluate the carcinogenic potential. For caspofungin, there were no effects on fertility in
studies conducted in male and female rats up to 5 mg/kg/day.

Sucrose

Mannitol
Glacial acetic acid
Sodium hydroxide (to adjust the pH)

Do not mix with diluents containing glucose, as Fungiska is not stable in diluents containing
glucose. In the absence of compatibility studies, this medicinal product must not be mixed with
other medicinal products.

For Fungiska 50 mg: 24 months For Fungiska 70 mg: 24 months Fungiska contains no preservatives. From a microbiological point of view, the product should be used immediately. If not used immediately, in use storage times and conditions prior to use are the responsibility of the user and would normally not be longer than 24 hours at 2 to 8°C or below 25°C, unless reconstitution and dilution have taken place in controlled validated aseptic conditions.

Unopened vials: store in a refrigerator (2°C - 8°C).
For storage conditions after reconstitution and dilution of the medicinal product, see section
6.3.

10 ml Type I glass vial with a rubber stopper and an aluminium flip-off cap.
Supplied in packs of 1 vial.

Reconstitution of Fungiska

DO NOT USE ANY DILUENTS CONTAINING GLUCOSE, as Fungiska is not stable in diluents containing glucose. DO NOT MIX OR CO-INFUSE Fungiska WITH ANY OTHER MEDICINES, as there are no data available on the compatibility of Fungiska with other intravenous substances, additives, or medicinal products. Visually inspect the infusion solution for particulate matter or discolouration.

 

Any unused medicinal product or waste material should be disposed of in accordance with local requirements.

INSTRUCTIONS FOR USE IN ADULT PATIENTS

Step 1 Reconstitution of conventional vials

To reconstitute the 50 mg powder, bring the vial to room temperature and aseptically add 10.5 ml of water for injection. The concentrations of the reconstituted vials will be 5.2 mg/ml.

 

To reconstitute the 70 mg powder, bring the vial to room temperature and aseptically add 10.5 ml of water for injection. The concentrations of the reconstituted vials will be 7.2 mg/ml.

 

The white to off-white compact lyophilised powder will dissolve completely. Mix gently until a clear solution is obtained. Reconstituted solutions should be visually inspected for particulate matter or discolouration. This reconstituted solution may be stored for up to 24 hours at or below 25°C.

 

Step 2 Addition of reconstituted Fungiska to patient infusion solution

Diluents for the final solution for infusion are: sodium chloride solution for injection, or lactated Ringer’s solution. The solution for infusion is prepared by aseptically adding the appropriate amount of reconstituted concentrate (as shown in the table below) to a 250 ml infusion bag or bottle. Reduced volume infusions in 100 ml may be used, when medically necessary, for 50 mg or 35 mg daily doses.

Do not use if the solution is cloudy or has precipitated.

 

PREPARATION OF THE SOLUTION FOR INFUSION IN ADULTS

DOSE*	Volume of reconstituted Fungiska for transfer to intravenous bag or bottle	Standard preparation (reconstituted Fungiska added to 250 ml) final concentration	Reduced volume infusion (reconstituted Fungiska added to 100 ml) final concentration
50 mg	10 ml	0.20 mg/ml	-
50 mg at reduced volume	10 ml	-	0.47 mg/ml
35 mg for moderate hepatic impairment (from one 50 mg vial)	7 ml	0.14 mg/ml	-
35 mg for moderate hepatic impairment (from one 50 mg vial) at reduced volume	7 ml	-	0.34 mg/ml
70 mg	10 ml	0.28 mg/ml	Not Recommended
70 mg (from two 50-mg vials)**	14 ml	0.28 mg/ml	Not Recommended
35 mg for moderate hepatic impairment (from one 70 mg vial)	5 ml	0.14 mg/ml	0.34 mg/ml

* 10.5 ml should be used for reconstitution of all vials.

** If 70 mg vial is not available, the 70 mg dose can be prepared from two 50 mg vials.

 

INSTRUCTIONS FOR USE IN PAEDIATRIC PATIENTS

Calculation of Body Surface Area (BSA) for paediatric dosing

Before preparation of infusion, calculate the body surface area (BSA) of the patient using the following formula: (Mosteller Formula)

Preparation of the 70 mg/m² infusion for paediatric patients >3 months of age (using a 50-mg vial)

1.        Determine the actual loading dose to be used in the paediatric patient by using the patient's BSA (as calculated above) and the following equation:

BSA (m²) X 70 mg/m² = Loading Dose

The maximum loading dose on Day 1 should not exceed 70 mg regardless of the patient's calculated dose.

2.        Equilibrate the refrigerated vial of Fungiska to room temperature.

3.        Aseptically add 10.5 ml of water for injection.^a This reconstituted solution may be stored for up to 24 hours at or below 25°C.^b This will give a final caspofungin concentration in the vial of 5.2 mg/ml.

4.        Remove the volume of medicinal product equal to the calculated loading dose (Step 1) from the vial. Aseptically transfer this volume (ml)^c of reconstituted Fungiska to an IV bag (or bottle) containing 250 ml of 0.9%, 0.45%, or 0.225% Sodium Chloride Injection, or Lactated Ringers Injection. Alternatively, the volume (ml)^c of reconstituted Fungiska can be added to a reduced volume of 0.9%, 0.45%, or 0.225% Sodium Chloride Injection or Lactated Ringers Injection, not to exceed a final concentration of 0.5 mg/ml. This infusion solution must be used within 24 hours if stored at 2 to 8°C or below 25°C.

 

Preparation of the 50 mg/m² infusion for paediatric patients >3 months of age (using a 50-mg vial)

1.        Determine the actual daily maintenance dose to be used in the paediatric patient by using the patient's BSA (as calculated above) and the following equation:

BSA (m²) X 50 mg/m² = Daily Maintenance Dose

The daily maintenance dose should not exceed 70 mg regardless of the patient's calculated dose.

2.      Equilibrate the refrigerated vial of Fungiska to room temperature.

3.      Aseptically add 10.5 ml of water for injection.^a This reconstituted solution may be stored for up to 24 hours at or below 25°C.^b This will give a final caspofungin concentration in the vial of 5.2 mg/ml.

4.      Remove the volume of medicinal product equal to the calculated daily maintenance dose (Step 1) from the vial. Aseptically transfer this volume (ml)^c of reconstituted Fungiska to an IV bag (or bottle) containing 250 ml of 0.9%, 0.45%, or 0.225% Sodium Chloride Injection, or Lactated Ringers Injection. Alternatively, the volume (ml)^c of reconstituted Fungiska can be added to a reduced volume of 0.9%, 0.45%, or 0.225% Sodium Chloride Injection or Lactated Ringers Injection, not to exceed a final concentration of 0.5 mg/ml. This infusion solution must be used within 24 hours if stored at 2 to 8°C or below 25°C.

 

Preparation of the 70 mg/m2 infusion for paediatric patients >3 months of age (using a 70-mg vial)

1. Determine the actual loading dose to be used in the paediatric patient by using the patient's BSA (as calculated above) and the following equation:

BSA (m²) X 70 mg/m² = Loading Dose

The maximum loading dose on Day 1 should not exceed 70 mg regardless of the patient's calculated dose.

2. Equilibrate the refrigerated vial of Fungiska to room temperature.

3. Aseptically add 10.5 ml of water for injection.^a This reconstituted solution may be stored for up to 24 hours at or below 25°C.^b This will give a final caspofungin concentration in the vial of 7.2 mg/ml.

4. Remove the volume of medicine equal to the calculated loading dose (Step 1) from the vial. Aseptically transfer this volume (ml)^d of reconstituted Fungiska to an IV bag (or bottle) containing 250 ml of 0.9 %, 0.45 %, or 0.225 % Sodium Chloride Injection, or Lactated Ringers Injection. Alternatively, the volume (ml)^d of reconstituted Fungiska can be added to a reduced volume of 0.9 %, 0.45 %, or 0.225 % Sodium Chloride Injection or Lactated Ringers Injection, not to exceed a final concentration of 0.5 mg/ml. This infusion solution must be used within 24 hours if stored at 2 to 8°C or below 25°C.

 

Preparation of the 50 mg/m2 infusion for paediatric patients >3 months of age (using a 70-mg vial)

1. Determine the actual daily maintenance dose to be used in the paediatric patient by using the patient's BSA (as calculated above) and the following equation:

BSA (m²) X 50 mg/m² = Daily Maintenance Dose

The daily maintenance dose should not exceed 70 mg regardless of the patient's calculated dose.

2. Equilibrate the refrigerated vial of Fungiska to room temperature.

3. Aseptically add 10.5 ml of water for injection.^a This reconstituted solution may be stored for up to 24 hours at or below 25°C.^b This will give a final caspofungin concentration in the vial of 7.2 mg/ml.

4. Remove the volume of medicine equal to the calculated daily maintenance dose (Step 1) from the vial. Aseptically transfer this volume (ml)^d of reconstituted Fungiska to an IV bag (or bottle) containing 250 ml of 0.9 %, 0.45 %, or 0.225 % Sodium Chloride Injection, or Lactated Ringers Injection. Alternatively, the volume (ml)^d of reconstituted Fungiska can be added to a reduced volume of 0.9 %, 0.45 %, or 0.225 % Sodium Chloride Injection or Lactated Ringers Injection, not to exceed a final concentration of 0.5 mg/ml. This infusion solution must be used within 24 hours if stored at 2 to 8°C or below 25°C.

 

Preparation notes:   a The white to off-white cake will dissolve completely. Mix gently until a clear solution is obtained. b Visually inspect the reconstituted solution for particulate matter or discoloration during reconstitution and prior to infusion. Do not use if the solution is cloudy or has precipitated. c Fungiska is formulated to provide the full labeled vial dose (50 mg) when 10 ml is withdrawn from the vial. d Fungiska is formulated to provide the full labeled vial dose (70 mg) when 10 ml is withdrawn from the vial.