You may be trying to access this site from a secured browser on the server. Please enable scripts and reload this page.
Turn on more accessible mode
Turn off more accessible mode
Skip Ribbon Commands
Skip to main content
Turn off Animations
Turn on Animations
Follow
Students
Alumni
Faculty
Media
Careers
Libraries
emp-2
It looks like your browser does not have JavaScript enabled. Please turn on JavaScript and try again.
University Hospitals
Examination Board
Careers
Libraries
Campuses & Sites
News
Events
Contact Us
Mother & Child Health Research & Training Centre, Matiari
About Us
Our Leadership
Our Publications
Contact Us
Research
Currently selected
Our Projects
Our Partners
Meet the Team
Resources
KNOWLEDGE SHARING
Trainings, Workshops & Seminars
Home
Mother & Child Health Research & Training Centre, Matiari
Mother & Child Health Research & Training Centre, Matiari
Research
Mother & Child Health Research & Training Centre, Matiari
About Us
Research
Currently selected
Our Projects
Our Partners
Meet the Team
Resources
Trainings, Workshops & Seminars
Experimental Medicine Platform-II
Principal Investigator:
Dr. Professor Asad Ali.
Co-PI:
Dr. Najeeha Iqbal, Dr. Junaid Iqbal, Dr. Zehra Jamil, Dr Sana Zahiruddin, Dr. Gulnaz Shafqat.
Funded by:
Bill and Melinda Gates Foundation.
Project Duration
: 24 months.
Project Sites
: Matiari and AKUH Karachi, Pakistan, Bangladesh, Zambia, and Burkina Faso.
Primary objectives
: To assess if administration of oral vancomycin followed by VE818 to pregnant women colonised with at least 2 out of 11 selected bacterial enteropathogens results in a significant change in the mean count of these organisms between the baseline and 2 weeks after completion of the intervention (Study Day 35d +2), compared to oral vancomycin followed by placebo.
Secondary Objectives
:
To assess the impact of VE818 on a panel of inflammatory biomarkers in pregnant women:
Plasma: CRP, AGP, sCD14, LBP, CD163, and iFABP
Fecal: myeloperoxidase, neopterin, calprotectin and lipocalin
To determine if VE818 in combination with vancomycin can reduce overall enteropathogen colonization in pregnant women compared to vancomycin alone
To determine engraftment of the bacterial species present in VE818 in pregnant women
To determine if VE818 can reduce intestinal permeability in pregnant women
To determine if VE818 can impact the structure and function of fecal, vaginal and oral microbiome in pregnant women
To determine if VE818 can impact the host metabolome in pregnant women.
