Diarrhea Clinical Trial
Official title:
Treatment and Prevention of Oral and Alimentary Mucositis Using Polymerized Cross-Linked High Potency Sucralfate as a Single Agent Therapy
RATIONALE: Polymerized (cross-linked) sucralfate malate paste (ProThelial) may be an
effective single therapy approach for the management of chemoradiation mucositis, treating
and preventing its occurrence in the oral cavity, esophagus, stomach, small and large
intestine.
PURPOSE: This observational multi-phase trial is studying how well polymerized
(cross-linked) sucralfate malate paste (ProThelial) works to prevent and treat mucositis in
adult patients who are to receive or have received chemo/radiation therapy that have caused
or is anticipated to cause mucositis in the oral cavity, esophagus, stomach, small or large
intestine. The Phase IV study addresses prevention and treatment in the oral cavity. The
Phase I study addresses prevention and treatment in the esophagus, stomach, small and large
intestine.
OBJECTIVES:
Primary
- Observe the incidence of mucositis in patients receiving ProThelial prior to developing
chemoradiation mucositis in the oral cavity, esophagus, stomach, small or large
intestine.
- Observe the change from baseline in symptoms & signs of mucositis in chemoradiation
patients on Prothelial who have developed mucositis in the oral cavity, esophagus,
stomach, small or large intestine.
Secondary
- Patient-reported quality of relief by ProThelial (treatment portion) Using Pain Visual
Analogue Scale (PVAS) Using Difficulty Swallowing Visual Analogue Scale (DSVAS)
- To evaluate the safety and tolerability of ProThelial (Phase I non-oral uses)
- To observe the adverse event profile of ProThelial using patient-reported Questionnaire
- To observe effect on pain assessed day 1, 2,4,7,14,21 by Pain VAS
- To observe effect on oral ulcerations assessed day 1, 2,4,7,14,21 by OMAS
- To observe effect on symptoms of esophageal mucositis assessed day1, 2,4,7,14, 21using
Difficulty Swallowing Visual Analogue Scale
- To observe effect on symptoms of gastric and small intestine mucositis assessed day
1,2,4,7,14,21 using the Nausea Visual Analogue Scale & the NCI GI Toxicity Scale for
Nausea, Vomiting
- To observe effect on symptoms of large intestine mucositis assessed day 1,2,4,7,14,21
by NCI GI Toxicity Scale for Colonic Diarrhea
Tertiary
- Functional status prior to and following use of ProThelial (ECOG/Karnofsky) in patients
with mucositis
OUTLINE:
This is a multicenter observation study with 3 treatment cohorts and 3 prevention cohorts.
Patients are stratified according to gender, age, treatment, cancer under treatment (type &
stage), the presence, type, & severity of mucositis.
- Treatment (active mucositis): Patients are grouped in accordance to the type of
mucositis experienced - oral/esophageal, gastric/small intestine & colonic.
- ▪ Arm 1 Patients with oroesophageal mucositis (with pain, erythema, ulceration and
difficult pain swallowing as prominent symptom/signs) (Phase I)
- ▪ Arm 2 Patients with gastric/small intestinal mucositis (delayed nausea vomiting as
prominent symptom/sign). (Phase I)
- ▪ Arm 3 Patients with chemoradiation diarrhea as their prominent symptom/sign. (Phase
I)
- Prevention (no mucositis): Patients are grouped in accordance to type of mucositis
anticipated - oral/esophageal, gastric/small intestine and colonic.
- ▪ Arm 4 Patients anticipated to develop oroesophageal mucositis (with pain, erythema,
ulceration and difficult pain swallowing as prominent symptom/signs). (Phase IV)
- ▪ Arm 5 Patients anticipated to develop gastric/small intestinal mucositis (delayed
nausea vomiting as prominent symptom/sign) (Phase I)
- ▪ Arm 6 Patients anticipated to develop chemoradiation diarrhea as their prominent
symptom/sign. (Phase I)
BACKGROUND ON INTERVENTION: PROTHELIAL™ Polymerized High Potency Sucralfate Malate Paste
STANDARD POTENCY VS HIGH POTENCY SUCRALFATE IN MANAGING MUCOSITIS
Standard potency non-polymerized sucralfate is not recommended by MASCC/ISOO (Multinational
Association of Supportive Care in Cancer/ International Society of Oral Oncology) for the
treatment or prevention of mucositis, oral or alimentary. However high potency polymerized
sucralfate has been associated with rapid amelioration and prevention of both oral and
alimentary mucositis in a patient with advanced head neck cancer treated simultaneously with
high dose chemo-radiation. High potency sucralfate is standard sucralfate polymerized into
'sucralfate sheets' that adhere and orderly layer upon the mucosa achieving and maintaining
elevated concentrations of sucralfate long after the initial dose administration. Three
hours following administration, high potency sucralfate maintains a 7 fold greater surface
concentration of sucralfate on normal lining and a 23 fold greater concentration on
inflamed, ulcerated mucosa. In August 2013, the FDA cleared the use of ProThelial, a
polymerized high potency sucralfate paste, as a device for the management of oral mucositis.
RAPID HEALING BY STANDARD POTENCY SUCRALFATE AT HIGH DOSES
Early sucralfate investigations showed that undissolved (thus high dose concentration)
sucralfate adherent to the human gastric mucosa caused rapid mucosal changes within 10-60
minutes. These changes included the release of mucus and bicarbonate as well as
vacuolization and exfoliation of superficial enterocytes being replaced by newly regenerated
cells. Laboratory animals given high doses of standard potency sucralfate (3-20 times the
standard 14mg/kg dose) were observed to resist gastric injury, rapidly heal mucosal injuries
and showed increased secretion of luminal prostaglandins, mucus and bicarbonate. These
mucosal changes were shown to be linked to the local expression of growth factor receptors
and the secretion of epidermal growth factor. Later research identified that
sucralfate-mediated mucosal changes are growth factor dependent. Independently investigators
have concluded that sucralfate accelerates growth-factor mediated mucosal healing, though
the mechanism is unclear.
RAPID HEALING BY HIGH POTENCY SUCRALFATE GIVEN AT LOW DOSES
High potency sucralfate is the active ingredient of ProThelial. At standard 14mg/kg doses,
high potency sucralfate causes a 7-23 fold hyper-concentration of sucralfate on mucosal
lining. In a placebo controlled, double blinded multi-center trial involving 60 patients,
there was a 28 day 87.7% healing rate of GERD erosions (compared to placebo's 37.7%) in
patients using high potency sucralfate at 1.5 gram twice daily. This represented a 2.34 fold
or 334% improvement in healing over placebo. Esophageal erosions in both treatment groups
were exposed to untreated gastric acid making the results observed with high potency
sucralfate that much more remarkable.
Similarly, in a randomized 7 day four-arm trial involving 41 patients with erosive GERD, the
rate of healing for patients using high potency sucralfate was 80%. The 7 day healing rate
for acid therapy groups were considerably lower: omeprazole (20mg bid) was 30% and for
ranitidine (150mg bid) and antacid groups healing was 0%. Apparently the topical coating of
high potency sucralfate affects a mucosa-centric mechanism for healing that appears
indifferent to gastric pH or acid exposure. Comparing the 7 day healing rate of high potency
sucralfate to that of omeprazole there was a 2.67 or 367% improvement similar to that seen
when high potency sucralfate is compared to placebo where there was a 2.34 fold or 334%
improvement.
EXPERIENCE USING HIGH POTENCY SUCRALFATE FOR ORAL & ALIMENTARY MUCOSITIS IN STAGE 4B HEAD
AND NECK CANCER
In a 42 yo head and neck patient treated simultaneously with paclitaxel, carboplatin and
radiation (201Gy), high potency sucralfate (HPS - ProThelial) prevented mucositis, allowing
continuance of standard oral diet. The percutaneous gastric-tube surgically placed in
anticipation of Grade 3-4 mucositis was never used by the patient. While on ProThelial, the
patient never developed mucositis. Noncompliant discontinuation of HPS by patient midway
through chemo-radiation led to the emergence oral and alimentary mucositis with oral
erythema, nausea and diarrhea. Two days following resumption of HPS, both oral and
alimentary mucositis disappeared. Throughout treatment with ProThelial a normal oral diet
was maintained and no analgesia was required for mucositis. Patient reported no adverse
events while on HPS for 6 weeks.
PROTHELIAL'S DEVICE MECHANISM OF ACTION - EXPEDITED HEALING
High potency sucralfate in polymerized sucralfate malate paste has a device mechanism of
action. It is assumed that the more efficient layering of polymerized sucralfate paste
produces adherent restrictive microenvironment across the mucosal lining which advantages
the activation of growth factor receptors by growth factor. Restrictive micro-environs
generated by cross-linked layers of polymerized sucralfate "crowds" free-moving growth
factor, limiting its random movements to "pockets" that overlie growth factor receptors.
Spatially limiting the movement of growth factor to the vicinity of its receptor heightens
the chances of receptor site activation. This device action leads to expedited healing.
PROTHELIAL'S DEVICE MECHANISM OF ACTION - REVERSING MUCOSA-BASED PAIN, NAUSEA, VOMITING &
DIARRHEA
The surface "pockets" of restrictive micro-environs created by Prothelial's unique layering
probably affect the flux of ions across mucosal receptors responsible for pain, nausea,
vomiting and neuro-secretory diarrhea. These specialized mucosal receptors triggered by
chemo-radiation maintain their state of activation by means of gated-ion fluxes across
surface membranes that face the lumen of the gut. It is probable that the same restrictive
micro-environs that crowd growth factors to the vicinity of their receptors also affect the
surrounding space available to membranes for ion-flux and exchange. Spatial limitation of
the immediate surface environment surrounding ion-gated receptors along the GI tract impact
the receptor's ability to perpetuate the ion fluxes required to keep the receptor "turned
on" or stimulated. Physically restrictive micro-environs surrounding membranes of stimulated
receptors exhaust the ions immediately available to it for exchange. This limits the ability
of the receptor to stay "on". The result is the quiescence of the membrane and the reduction
of receptor-associated pain, nausea (thereby vomiting) and neurosecretory diarrhea, all of
which are triggered by chemoradiation therapy.
;
Observational Model: Cohort, Time Perspective: Prospective
Status | Clinical Trial | Phase | |
---|---|---|---|
Completed |
NCT06283784 -
Study To Evaluate The Efficacy of a Proprietary Mix of Live Probiotics In The Prophylaxis Of Diarrhea In Adult Patients
|
N/A | |
Recruiting |
NCT03851835 -
Multi-DOSE Oral Ondansetron for Pediatric Acute GastroEnteritis
|
Phase 3 | |
Completed |
NCT04003181 -
The Pathogenesis of Chronic Diarrhoea After Treatment for Cancer in Cecum and the Ascending Colon
|
N/A | |
Completed |
NCT03596827 -
The Protective Immune Response to Attenuated Enterotoxigenic Escherichia Coli Infection
|
N/A | |
Recruiting |
NCT05372068 -
Cement flooRs AnD chiLd hEalth (CRADLE)
|
N/A | |
Completed |
NCT03972618 -
Evaluation of the Efficacy of Sawyer Point One Filters in Schools and Homes in the Dominican Republic
|
N/A | |
Completed |
NCT05207618 -
Utility of the Administration of Chesnut and Quebracho Extract for Irritable Bowel Syndrome Diarrhea Predominant
|
N/A | |
Not yet recruiting |
NCT05052489 -
Registry and Clinical Observation of Children With Diarrhoeal Disease
|
||
Completed |
NCT02541695 -
Characterization of Resistance Against Live-attenuated Diarrhoeagenic E. Coli
|
N/A | |
Completed |
NCT02428647 -
Lao Zinc Study: Effects of Two Forms of Daily Preventive Zinc Versus Therapeutic Zinc Supplementation
|
N/A | |
Completed |
NCT02197780 -
Head-to-head Comparison of Two Fecal Biomarkers to Screen Children for IBD
|
N/A | |
Completed |
NCT01739231 -
Live Attenuated ETEC Vaccine ACE527 With and Without dmLT Adjuvant in Adults
|
Phase 1/Phase 2 | |
Completed |
NCT01968408 -
Lactobacillus Reuteri DSM 17938 in Preventing Nosocomial Diarrhea in Children
|
Phase 3 | |
Terminated |
NCT01472211 -
Water-based Zinc Intervention Trial in Zinc Deficient Children
|
Phase 0 | |
Completed |
NCT01371656 -
Levofloxacin in Preventing Infection in Young Patients With Acute Leukemia Receiving Chemotherapy or Undergoing Stem Cell Transplantation
|
Phase 3 | |
Not yet recruiting |
NCT01382199 -
Recombinant Human Lactoferrin Administered Orally for the Prevention of Antibiotic Associated Diarrhea in Adult Patients
|
Phase 3 | |
Completed |
NCT01438645 -
ScopeGuide-assisted Colonoscopy Versus Conventional Colonoscopy
|
N/A | |
Terminated |
NCT01048567 -
Efficacy and Safety of Lactobacillus Acidophilus/Rhamnosus Combination for the Prevention of Antibiotic-associated Diarrhea in the Elderly
|
Phase 2 | |
Completed |
NCT00914225 -
Effect of Bednets and a Water Purification Device on HIV Disease Progression Among ART naïve Patients in Kenya
|
N/A | |
Completed |
NCT00760851 -
Yogurt Study in Children 2-4 Years Old Attending Daycare
|
Phase 3 |