PMID- 20648928
OWN - NLM
STAT- MEDLINE
DCOM- 20100921
LR  - 20220321
IS  - 0004-4172 (Print)
IS  - 0004-4172 (Linking)
VI  - 60
IP  - 6a
DP  - 2010
TI  - Pharmacokinetics, safety and tolerability of intravenous ferric carboxymaltose: a 
      dose-escalation study in volunteers with mild iron-deficiency anaemia.
PG  - 362-72
LID - 10.1055/s-0031-1296301 [doi]
AB  - Iron-deficiency anaemia (IDA) represents a major burden to public health 
      worldwide. The therapeutic aim for patients with IDA is to return iron stores and 
      haemoglobin (Hb) levels to within the normal range using supplemental iron 
      therapy and erythropoiesis-stimulating agents. Oral and previous intravenous 
      (i.v.) iron formulations have a number of disadvantages, including immunogenic 
      reactions, oxidative stress, low dosages, long administration times and the 
      requirement for a test dose. Ferric carboxymaltose (FCM, Ferinject) is a novel, 
      next-generation i.v. iron formulation with the potential to overcome these 
      limitations. In this single-centre, randomized, double-blind, placebo-controlled 
      study, the pharmacokinetics (PK), pharmacodynamics (PD), safety and tolerability 
      of single, escalating doses of FCM were investigated. Four ascending doses were 
      investigated in a total of 24 patients with mild IDA (defined as serum ferritin < 
      20 microg/l and transferrin saturation [TfS] < 16%): 100 mg iron as FCM given as 
      an i.v. bolus injection, and 500, 800 and 1000 mg iron as FCM given as an i.v. 
      infusion over 15 min. At each dose level six patients received FCM and two 
      received placebo. The decision to escalate to the next dose was based on 
      evaluation of safety and tolerability data from the previous dose. The maximum 
      duration of the study was 5 weeks from screening to final assessment. Assessments 
      were made of PK iron-status parameters up to 168 h post-dose. Safety assessments 
      included incidence of adverse events (AEs), clinical laboratory parameters and 
      vital signs. PK and PD parameters were analysed using descriptive statistics. All 
      analyses were performed on the safety population, which included all patients who 
      received > or = 1 dose of study medication. Seventy-seven patients were screened 
      and, of these, 32 male and female patients with pre-study Hb between 9.2 and 11.9 
      g/dl and serum ferritin < 20 microg/l were included in the study. Two patients 
      had TfS > 16% (19.2% and 17.2%); both patients were considered by the 
      investigator to be eligible for inclusion. Compared with placebo, a rapid, 
      dose-dependent increase in total serum iron was observed across all dose groups. 
      Mean (standard deviation) maximum total serum iron levels ranged between 36.9 
      (4.4) and 317.9 (42.3) microg/ml in the 100 and 1000 mg groups. 
      Concentration-time curves of total serum iron continuously declined for up to 24 
      and 72 h post-dose in the 100 and 500-1000 mg groups, respectively. 
      Non-compartmental analysis of PK parameters was truncated at 24 h (100 mg) and 72 
      h (500-1000 mg doses). A dose-dependent, but not dose-linear, increase in serum 
      ferritin was seen in all treatment groups compared with placebo, with peak levels 
      of a 23-210-fold increase above baseline occurring 48-120 h postdose. 
      Iron-binding capacity was transiently almost fully utilized after doses of 500, 
      800 and 1000 mg (TfS > 95%). No meaningful changes in serum transferrin or serum 
      transferrin receptor concentrations were observed during this study. The 
      elimination pattern for FCM appeared to be mono-exponential; FCM was cleared from 
      serum with a terminal halflife of approximately 7.4-12.1 h. The percentage of FCM 
      excreted in urine was negligible (0.0005%). FCM was well tolerated; a total of 19 
      AEs were reported by 8/32 patients (25%), of which three were considered by the 
      investigator to be related to FCM: nausea and vomiting (one patient [100 mg]), 
      and headache (one patient [1000 mg]). The incidence of AEs did not increase with 
      dose. No severe or serious AEs, or deaths occurred. FCM had no significant effect 
      on laboratory safety parameters or vital signs. This study satisfactorily 
      characterized the PK/PD parameters of single doses of 100, 500, 800 and 1000 mg 
      iron as FCM. The majority of FCM was utilized or eliminated within 24 h of 
      administration of a 100 mg dose and within 72 h of a 500-1000 mg dose. FCM was 
      generally well tolerated across all doses in patients with mild IDA.
FAU - Geisser, Peter
AU  - Geisser P
AD  - Vifor (International) Inc., St. Gallen, Switzerland. 
      peter.geisser@viforpharma.com
FAU - Banke-Bochita, Jose
AU  - Banke-Bochita J
LA  - eng
PT  - Journal Article
PT  - Randomized Controlled Trial
PT  - Research Support, Non-U.S. Gov't
PL  - Germany
TA  - Arzneimittelforschung
JT  - Arzneimittel-Forschung
JID - 0372660
RN  - 0 (Ferric Compounds)
RN  - 6897GXD6OE (ferric carboxymaltose)
RN  - 69-79-4 (Maltose)
SB  - IM
MH  - Adolescent
MH  - Adult
MH  - Anemia, Iron-Deficiency/*drug therapy
MH  - Blood Pressure/drug effects
MH  - Body Temperature/drug effects
MH  - Dose-Response Relationship, Drug
MH  - Double-Blind Method
MH  - Electrocardiography
MH  - Female
MH  - Ferric Compounds/administration & dosage/*pharmacokinetics/therapeutic use
MH  - Heart Rate/drug effects
MH  - Humans
MH  - Infusions, Intravenous
MH  - Male
MH  - Maltose/administration & dosage/*analogs & 
      derivatives/pharmacokinetics/therapeutic use
MH  - Middle Aged
EDAT- 2010/07/23 06:00
MHDA- 2010/09/23 06:00
CRDT- 2010/07/23 06:00
PHST- 2010/07/23 06:00 [entrez]
PHST- 2010/07/23 06:00 [pubmed]
PHST- 2010/09/23 06:00 [medline]
AID - 10.1055/s-0031-1296301 [doi]
PST - ppublish
SO  - Arzneimittelforschung. 2010;60(6a):362-72. doi: 10.1055/s-0031-1296301.