BMI Clinical Trial
Official title:
Evaluation of Skin, Colonic and Oral Microbiota and Effect of Time and Antibiotic Treatment on Organism Diversity at Each Site
Background:
- Most studies of infectious agents have focused on specific microbes, such as human
papillomaviruses and cervical cancer, and the hepatitis B and C virus and liver cancer.
The skin and many internal areas (including the mouth and the gastrointestinal tract)
also contain large numbers of naturally occurring microbes, but these areas have not
received as much study.
- Some of the infectious agents that naturally reside in the body may have an effect on
health. The study of naturally occurring microbes in the human body is a new area of
research, and much remains to be learned regarding the extent and pattern of their
appearance and appropriate techniques for testing them.
- Researchers are interested in collecting human samples from areas known to contain
naturally occurring microbes. These samples will provide baseline information for
further studies.
Objectives:
- To collect a set of study samples from individuals who have applied to participate in a
study assessing the relationship among the bacteria H. pylori, peptic ulcer disease, and
gastric cancer.
Eligibility:
- Individuals between the ages of 21 and 65 who are participating in the clinical trial
entitled A Phase III Randomized Trial of Three Antibiotic Regimens to Eradicate Helicobacter
Pylori.
Design:
- Researchers will collect oral (saliva), colonic, and skin swab samples from study
participants who tested positive for the presence of the H. pylori bacteria. These
samples will be collected at the three study visits (enrollment, 6 weeks, and 1 year).
- Researchers will also collect samples from people who applied for the clinical trial but
did not test positive for H. pylori. These samples will be collected at the enrollment
visit and 1 year later.
- Blood samples will be collected at each study visit.
The study of infectious agents and their role in disease is not new. Most efforts in this
area have focused on specific agents, such as human papillomaviruses and cervical cancer,
Helicobacter pylori (HP) and gastric diseases and carcinoma, hepatitis B and C virus and
liver cancer, to name a few. The body s skin and mucosal surface s play host to microbial
communities (the microbiome) whose membership outnumbers our own somatic and germ cells by an
order of magnitude or more. The skin, oral, and gastrointestinal (GI) tract are all densely
colonized surfaces . Recent technological advances, however, have made exploration of the
microbiome, an understudied area, feasible. It is reasonable to hypothesize that some of the
infectious agents that naturally reside in the body may impact health, or that perhaps the
balance between the various micro-organisms has an effect on health. This new field of study
has much promise that could lead to important new discoveries of how infectious agents are
associated with disease and how environmental (e.g., diet) and host responses (e.g., immune
response and genetics) to these agents determine chronic patterns of colonization and
subsequent disease risk.
However, because the study of the human microbiome is a new area of research, much remains to
be learned regarding: a) the extent and pattern of the microbiome at various sites, b)
determinants of these patterns (e.g., consistency over time), and c) optimal assay
techniques.
Prior to launching large-scale epidemiological studies to evaluate the association between
microbiome and disease (including cancer), it is crucial to conduct well-designed,
systematic, methodological studies to address some of the issues listed above. These
methodological studies will begin to provide the baseline information that could be used to
plan for, and conduct disease association studies.
We propose to initiate a study to collect oral, skin, vaginal (only women), penile (men only)
and colonic samples at enrollment and again 6 months later on up to 150 individuals. Our
objectives are:
1. To evaluate the microbiome heterogeneity between individuals across specimen types -
colonic/oral/skin/vaginal/penile.
2. To evaluate the microbiome heterogeneity within individuals (over time and across
specimen types - colonic/oral/skin/vaginal/penile).
3. To evaluate the effect of self-reported antibiotic treatment on the oral, colonic, skin,
penile and vaginal microbiomes diversity and richness.
4. To evaluate the associations between colonic microbiome and gastrointestinal symptom
disorders (assessed by the Rome III questionnaire - a detailed diagnostic questionnaire
for adult functional gastrointestinal disorder), inflammatory markers (initially using
measures of C-reactive protein (CRP)), and demographic factors.
5. To evaluate the reproducibility of assays used to measure the microbiota and compare the
diversity and abundance determined by the different assays.
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