Ulcerative Colitis Clinical Trial
Official title:
A Pilot, Open-label, Multi-center Clinical Trial to Investigate the Safety and Efficacy of Bovine-Calf Intestinal Alkaline Phosphatase in Patients With Moderate to Severe Ulcerative Colitis.
Ulcerative colitis is characterized by abnormal activation of, and damage to, the colon epithelium, which is considered to be a central pathogenic mechanism. Activation of colon epithelium cells in UC is associated with an abnormal high expression of Toll-like receptors, including TLR-4, the major transducer of LPS, binding specifically the lipid A portion of LPS. Alkaline Phosphatase binds and subsequently dephosphorylates LPS, thereby eliminating the ability of LPS to activate TLR-4. This is expected to 1) prevent activation of the intestinal epithelium and 2) prevent systemic inflammatory responses that result from transmigration of endotoxin though the leaky inflamed intestinal mucosa. Therefore, it is expected that administration of BIAP may attenuate or prevent the local and systemic inflammatory response in patients with severe ulcerative colitis.
Inflammatory Bowel Disease (IBD) is a general term for a group of non-specific, chronic
inflammatory disorders of the digestive tract, of unknown etiology. IBD may be divided in
two major categories: Ulcerative colitis and Crohn's disease, both characterized by a
tendency towards frequent acute relapses leading to devastating chronic destruction of the
intestinal mucosal barrier function. Whereas Crohn's disease can affect the whole digestive
tract, ulcerative colitis is characterized by colonic involvement only. Surgical
intervention is frequently required in both Crohn's disease and ulcerative colitis.
Therapeutic intervention to date predominantly is based on reduction of induced local
mucosal- or systemic inflammation by the use of 5-ASA, corticosteroids, cyclosporine, or
TNFα antibodies.
In IBD, the delicate balance between pro-inflammatory molecules, anti-inflammatory molecules
and immunoregulatory cells, which tightly regulate the immune system, is disrupted and this
results in chronic, relapsing inflammation. Tissue and plasma concentrations of
pro-inflammatory cytokines such as IFN-gamma, IL-1ß, IL-6, IL-8 and TNFα are elevated in
inflammatory bowel disease and correlate with IBD activity.
In patients with inflammatory bowel diseases circulating LPS have been detected and also
increased AP levels have been observed. The presence of the endotoxin is probably the
consequence of the damaged intestinal mucosa leading to an increased LPS influx or gut
translocation and causing or aggravating the systemic inflammatory response. The increased
AP levels observed in these patients may be caused by the suboptimal detoxification of the
gut-derived influx of LPS and a response thereof of non-intestinal organs. Thus it has been
proposed that the liver sheds alkaline phosphatase (fast acting liver alkaline phosphatase)
massively after having been insulted with LPS.
Systemic consequences of IBD may be induced and/or aggravated significantly by the influx of
LPS. The proposed normal natural defense mechanism against LPS does include, amongst others,
the cleavage of one of the phosphate groups from LPS by endogenous AP. It is therefore
conceivable that a reduction in the amount of active LPS in the intestinal lumen by
exogenously administered AP will result in a corresponding relative decrease of LPS-influx
in the circulation of a subject and, as a consequence, inhibit the LPS medicated systemic
inflammatory response. Moreover, dephosphorylated LPS will reduce the ability of LPS to
activate TLR-4, resulting in decreased nuclear factor κB activation and a decreased local
inflammatory response.
In order to investigate the clinical potential of exogenously administered BIAP for human
use, its safety, tolerability and pharmacokinetics have previously been studied in animal
toxicology studies and in subsequent Phase I and IIa clinical trials, respectively. These
studies were done with intravenously administered BIAP. Following these studies and the
successful completion of animal pharmacology studies and a human volunteer study with oral
AP the next phase in the development of exogenously administered oral AP is to test the
compound in a limited population of patients with IBD.
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Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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