Shigellosis Clinical Trial
Official title:
Therapeutic Induction of Endogenous Antibiotics for Improved Recovery in Shigellosis
Shigellosis is one of the major causes of morbidity and mortality in many developing countries. The continued emergence of antibiotic resistant strains has complicated the treatment of shigellosis and has increased the cost of treatment markedly. Antimicrobial peptides are considered as endogenous antibiotic. A mixture of these antimicrobial peptides (LL-37 and beta-defensin) drenches the mucosal epithelial surfaces forming a barrier for invading microorganisms. Recently, we found that Shigella down-regulates the expression of LL-37 and beta-defensin 1 (HBD-1) in the colon of patients during acute shigellosis thereby facilitating bacterial invasion. Both LL-37 and HBD-1 could inhibit the growth of various microbes e.g. S. dysenteriae type 1, S. flexneri, and S. boydii. Our study indicated that bacterial DNA might be a potential mediator for the down- regulation in vitro. Down-regulation of LL-37 and HBD-1 was also seen in watery diarrhea caused by other pathogens. Thus, bacteria-mediated down-regulation of our front line defenses could be one strategy evolved by the pathogens to subvert this host-defense mechanism. gene encoding LL-37 in cultured epithelial cell lines were up-regulated when treated with butyrate; butyrate decreased the severity of Shigella infections in rabbit model. We could reproduce our findings from human i.e. downregulation of CAP-18 (the rabbit homologue to human LL-37) in colon epithelia after infection with Shigella flexneri. CAP-18 reappeared after treatment of the infected rabbits with sodium butyrate. Thus, the rabbit model demonstrated the proof of principal. In this study, we aim to assess the efficacy of sodium butyrate enema in reduction of clinical symptoms and / severity, reduction of inflammatory responses and induction of endogenous antibiotic activity in the rectum in adult patients with shigellosis.
Study design: A double blind randomized clinical trial with subsequent follow-up.
Study Subjects: Adult male and female patients attending the Clinical Research and Service
Center (CRSC) of ICDDR,B and Matlab Hospital will be screened for participation in the study.
Randomization:
According to a computer-generated randomization list, patients full filling the entry
criteria will be randomized to either intervention group (Pivmecellinam plus butyrate enema)
or control group (Pivmecellinam plus normal saline enema). Butyrate enema will contain 80
mmol/L of butyrate in normal saline (pH 7.2). Placebo enema will contain normal saline(pH
7.2)
Case management:
After enrollment, the patients will be admitted in the study ward of ICDDRB Dhaka and Matlab
hospital. A standard clinical history and clinical examination will be performed by one of
the investigators or study physician. All patients will receive Pivmecillinam, 400 mg, 8
hourly for 5 days. The intervention group will receive butyrate enema 80 ml of 80 mM sodium
butyrate, 12 hourly for 72 hours while the placebo group will get 80 ml of normal saline 12
hourly for 72 hours. All patients will receive the usual hospital food three times a day
(breakfast, lunch and supper). The patients will remain in the study ward for 5 days to
enable identification of any relapse cases.
Procedure for butyrate enema:
Patients will be instructed to lie on a bed (cholera cot) in left lateral position. A soft
rectal catheter will be introduced by a nurse/physician, through which 80 ml of butyrate
solution will be instilled slowly with a 50 ml plastic syringe. Patients will be asked to
retain the enema for at least ½ hour by remaining supine for 30 minutes after the
administration. However, if a patient cannot retain the enema for 30 minutes, he will be
given a second round of enema immediately after defecation.
Definition of clinical cure: A patient will be defined as clinically cured if on day-3, no
blood or mucus is observed in the stool, there is ≤ 3 unformed stool in 24 hours and no fever
(oral temperature > 37.5° C) is recorded.
Treatment failure: A patient will be considered a treatment failure on day 3 when there is
any one of the following features present: > 3 unformed stool in 24 hours, presence of blood
in any stool or presence of fever (oral temperature > 37.5° C).
Collection of Samples:
Patients will be requested to stay in the hospital for at least 5 days to facilitate disease
monitoring and sampling. On admission day (patients will be enrolled after serological
confirmation by slide agglutination test on the subsequent day i.e. day-1), stool specimens
will be collected from each patient every day starting from the day of admission till 4 days
after admission. Rectal biopsy samples will be collected on the day of admission and 7 days
after admission from patients enrolled in Dhaka hospital only. Three mL blood will be
collected after admission for measurement of C-reactive protein (CRP) that will be used as an
indicator for monitoring magnitude of inflammation. 1 mL blood from patients will be
collected to measure CRP in serum on the 4th day of admission.
Stool: Fresh stool samples will be collected for routine microscopic examination for
parasites or cysts and as well as RBC, pus cells and macrophages. Stool samples will also be
tested for measuring bacterial counts/load. In brief, 1 g of stool will be diluted in normal
saline (1:10), vortex-mixed for 5 min, followed by serial dilutions of 1:10 in normal saline
and plated in MacConkey agar plates. After overnight incubation at 37ºC, bacterial cfu will
be counted. Fresh stool specimens will also be extracted as described earlier for measuring
LL-37,human beta-defensin 1 and 3 and proinflammatory cytokines (interleukin-8 and 1beta) by
ELISA method.
Rectal biopsy: Rectal biopsy samples will be obtained from patients (only in Dhaka Hospital).
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