Inflammatory Bowel Disease Clinical Trial
Official title:
A Randomised Controlled Trial Comparing the Efficacy of Intravenous Iron Sucrose and Oral Iron Sulfate in Patients With Iron Deficiency.
Primary Hypothesis: There is no difference in the efficacy of iron replacement by oral or
intravenous route in Inflammatory Bowel Disease patients.
Iron deficiency anaemia is a common problem in people with inflammatory bowel disease (IBD)
and patients with excessive blood loss from the bowel or heavy menstrual loss. Treatment
options include a blood transfusion, oral iron with (Ferrograd ®) or intravenous iron
replacement with iron sucrose (Venofer®). Iron deficiency anaemia is associated with poor
quality of life, poor concentration span and low energy level. Blood transfusion may improve
symptomatic anaemia quickly but there is a risk of transfusion reaction and blood born
infection transmission. Moreover, packed cells are scarce resource therefore its use needs
to be carefully prioritized. Oral iron supplement has been widely used and it can be
purchased over the counter, however, its efficacy is not known in IBD population. Oral iron
is poorly tolerated with side effects include altered bowel habit, nausea and darken stools,
making it difficult to adhere to. In contrast, intravenous iron therapy with Venofer® has
been shown to replenish iron store and improve anaemia quickly. To date, the safety of
Venofer® use has been supported by its post marketing surveillance. Limitations with
intravenous iron replacement include the need for medical supervision in the setting of
limited healthcare resources; the need for patients to take multiple days off work and the
cost of Venofer®. Currently it is uncertain which method of iron replacement is better. The
purpose of this study is to compare the efficacy and the cost of oral and intravenous iron
replacement in the setting of iron deficiency anaemia.
1.1 Literature
Iron deficiency anemia is a common and a major management issue in Inflammatory Bowel
disease [1-3]. Moreover, no factor has been identified in predicting recurrent iron
deficiency anemia [4]. Iron deficiency and anemia are well recognized causes of fatigue,
poor concentration and decreased energy level which impact on one's quality of life and
ability to maintain employment or managing activities of daily living [2, 5]. Iron
deficiency anemia is multi-factorial in origin and its causes can be divided into disease or
patient origin. Disease factors include active blood loss from gastrointestinal mucosal
ulceration, impairment of iron absorption if disease affects the proximal small bowels or a
history of extensive small bowel resection. Iron absorption and utilization may also be
influenced by inflammation inducible production of the hepatic origin peptide hormone called
hepcidin [5], Interleukin 10 (IL10) [6] and interleukin 6 (IL 6) [7, 8]. Inflammatory
cytokines such as Tumour Necrosis Factor alpha (TNFa) and IL-6 have been shown to cause
anorexia in the animal model [9]. The major patient factor is dietary aversion of certain
food in order to avoid exacerbation of existing symptom [10, 11].
Iron can be replaced either orally or intravenously. To date five studies directly compare
oral versus intravenous iron therapy in patients with inflammatory bowel disease. Three of
the studies suggested intravenous iron was superior [12-14], one suggested oral iron was
superior [15]and one showed no difference[16]. This confusion is evident by a retrospective
review of a gastroenterology outpatient clinic's experience in detecting and managing iron
deficiency anaemia in both IBD and non IBD patients[17]. Furthermore, there are studies
advocating the concurrent use of Erythropoietin which makes it difficult to draw a definite
conclusion.
Studies have shown that iron deficient without anaemia is associated with reduced cognitive
performance and it is reversible with iron supplementation.(18)19) In combination with other
non specific symptoms such as fatigue and poor concentration span, many clinicians have been
treating iron deficiency before anaemia occurs. Moreover, the World Health Organization
(WHO) estimated the number of iron deficient people to be twice that of diagnosed anaemic
people, (20) therefore, it is more appropriate to use iron deficiency as the inclusion
criterion. This is in contrast with most of the clinical trials examining iron replacement
therapy use iron deficiency anaemia as the inclusion criteria. The approach of stratifying
the route of iron replacement therapy by the degree of anaemia is logical but not evidence
based. This study seeks to investigate the efficacy of intravenous iron versus oral iron
replacement in iron deficient patients.
Bone marrow biopsy staining for iron store is the gold standard for assessing iron store but
it is invasive, therefore surrogate serum markers such as ferritin and iron saturation are
used in clinical practice and they have been shown to be accurate.(21) Low ferritin level is
associated with high (78%-100%) specificity and low iron saturation has a high sensitivity
for iron deficiency (59%-88%). (22) Moreover, in anaemic IBD population, low ferritin level
has >90% specificity for iron deficiency. (23) Given some of the IBD patients will have
'functional' iron deficiency with elevated ferritin and CRP and a low iron saturation, we
have decided to use iron saturation <16% and ferritin less than 100ug/L to indicate iron
deficient state. This cut off is consistent with the laboratory standard for University of
Alberta Hospital.
1.2 Oral Iron Therapy
1.2.1 Oral Iron Adverse Events
Oral iron replacement is often poorly tolerated as evident by published studies where the
adverse reaction rate has been reported to be as high as 80% [12], the discontinuation rate
of up to 25% [16, 18]. Less than half of the patients were able to tolerate the prescribed
dose of oral iron [14]. Some reports suggested oral iron therapy is associated with
worsening of IBD disease activity [12], although not consistently [14]. Finally, there is
controversy regarding whether or not oral iron replacement could exacerbate underlying
disease through increased oxidative stress [18].
1.2.2. Oral Iron Efficacy
Semrin et al have demonstrated oral iron absorption is significantly impaired in the context
of active Crohn's disease when compared to inactive disease state [7]. In the literature,
the efficacy of oral iron replacement is often defined by an improvement in haemoglobin
level by 20g/L or more from baseline and it has been reported to be as high as 89% [15]. It
is worth noting that the baseline haemoglobin in the oral replacement cohort of the study by
Gisbert et al was significantly higher than the intravenous cohort. When using iron studies
as an endpoint, only 60% of oral iron treatment group were not iron deficient after 5 months
of as tolerated dose of oral iron replacement [14].
1.3 Intravenous Iron Therapy
1.3.1 Intravenous Iron Adverse Events
The alternative to oral iron is intravenous iron replacement and its formulation has changed
over time. Chertow et al reviewed the US FDA intravenous iron adverse event data between
2001-2003 and confirmed a up to 20 times higher rate of life threatening adverse events with
the high molecular weight iron dextran than iron sucrose [19]. Iron sucrose (1.4+/- 0.5g)
has been shown to increase HB by 20g/L and/or normalizing haemoglobin in up to 91% of the
cohort within 12 weeks of treatment [20]. Studies have shown intravenous iron therapy is
better tolerated than oral iron, with a lower discontinuation rate [13] and a definite
improvement in the serum ferritin [16]. Intravenous iron replacement ensures adequate total
iron replacement because there isn't an issue with compliance and it is independent from
intestinal absorption. Iron sucrose has been shown to be efficacious when oral iron
replacement is inadequate or intolerable [20]. The disadvantages of intravenous iron include
it being time consuming for the patient, much more expensive than the oral formulation and
the ancillary cost. It is uncertain what the true cost of intravenous iron replacement is
without factoring in efficacy, compliance and the lack of side effect. Intravenous iron
usage has been shown to be cost effective in chronic renal failure patients on dialysis who
has insufficient iron stores on maximum tolerated oral supplements [21].
1.3.2 Intravenous Iron Efficacy
There have been five direct comparative oral versus intravenous iron replacement studies.
The earlier comparative study involved smaller number of subjects, 19 patients, with short
treatment duration of 2 weeks [12] and 6 weeks [16] and in one study, the baseline entry
criterion between the two groups were different [15]. Appendix one summarises these studies.
1.4 Potential Aggravating Effects of Iron Therapy on Inflammatory Bowel Disease.
The role of oral iron in causing intestinal oxidative stress and subsequently increase the
risk of colorectal dysplasia is a controversial one. Lund et al used 18 healthy volunteers
to demonstrate that unabsorbed dietary iron is associated with a 40% increase in stool free
radicals formation and carcinogens production [22]. The hypothesis that dietary iron can
serve as a catalyst in the formation of highly reactive radical via the Fenton reaction [23,
24] and thereby causing cellular damage [25] and contributing to carcinogenesis has been
demonstrated in animal models [26, 27]. A more recent mice model by Seril et al demonstrated
the superiority of an intraperitoneal iron supplementation in replenishing splenic iron
store without an increase in colorectal dysplasia rate compared to mice fed oral iron
supplements [28]. Interestingly, there are conflicting reports regarding the role of
intravenous iron replacement and the increase in plasma oxidative stress [12, 29] and the
significance of this data is unknown. Currently, limited human literature is available
addressing this issue.
HYPOTHESIS:
Primary:
There is no difference in the efficacy of iron replacement by oral or intravenous route in
IBD patients.
Secondary:
There is no difference in the tolerability of oral and intravenous iron therapy.
The route of iron replacement does not impact on the colonic bacterial flora composition,
the underlying IBD state and the oxidative stress of the colonic mucosa as determined by
colonic biopsies analyzing for endoplasmic reticulum stress.
Oral iron replacement therapy is a cheap and efficacious way of replacing iron compare to
intravenous replacement.
2 Trial Design
2.1 Primary Endpoint Change in iron saturation at week 8 post initiation of treatment.
2.2 Secondary Endpoints
To describe the change in haemoglobin, ferritin, IBDQ, HBI and partial MAYO score in
patients before and after iron replacement.
To describe the changes in the colonic endoplasmic reticulum as an indicator of oxidative
stress.
To describe the changes in urinary metabolomics from iron replacement To describe the change
in the faecal bacteria composition pre and post iron replacement.
2.3 Study Design/Type
Open label Randomised Control Trial and observer blinded.
2.4 Randomization
Eligible all comers will be randomized into either IV or PO iron therapy in a 1:1 ratio.
Randomization will be performed externally and hold by EPICORE centre. EPICORE centre will
maintain the randomization code.
3.1 Trial Treatment/ Duration
3.2 Dose determination:-
Total amount of intravenous iron given is calculated by Ganzoni Equation:
Iron dose (mg) = body weight (kg) x (ideal Hb - actual Hb) x 0.24 + 15mg/kg of iron depot
3.3 Iron Sucrose: Administered by IV infusion (dilute 5 mL (equiv. Fe 100 mg) in 100ml of
NaCl 0.9%). Maximum amount of iron sucrose is 300mg per infusion per week.
3.4 Oral iron: 200mg equivalent of elemental iron is given twice a day for 3 months.
3.5 Discontinuation if
- withdrawal of consent
- Significant adverse event such as hypersensitivity reaction, dyspnoea and myalgia with
iron sucrose. (see appendix 2)
- Recurrent intolerable non hypersensitivity reaction such as fatigue and GI disturbance.
3.6 Product Accountability Iron tablet pill count will take place during the monthly review.
3.7 Data Identification Appendix 3: Trial activity Schedule.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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