1. The Human Microbiome Brian Koll, MD, FACP, FIDSA Professor of Medicine
ICAHN School of Medicine at Mount Sinai
Mount Sinai Health System Executive Director For
Infection Prevention
April 8, 2014

2. Outline of Talk The Human Microbiome Project
C. difficile and Fecal Microbiome
Fecal Transplant and the Microbiome
Cost Effectiveness of Fecal Transplant with Restoration of the Microbiome

3. Human Microbiome Project
United States National Institutes of Heath
Five year project
Identify and characterize the microorganisms which are found in association with both healthy individuals and those with diseases (the human microbiome)
Second phase
Explore the relationship between disease and changes in the human microbiome

4. Human Microbiome Project
Metagenomics
Genetic makeup of microbial communities from various body sites
Whole genome sequencing
Individual bacterial species
16S rRNA sequences amplified by PCR
Five body sites
Oral
Skin
Vagina
Gut
Nasal/Lung

5. Human Microbiome Project

6. Human Microbiome Project

7. Human Microbiome Project

8. Human Microbiome Project

9. Human Microbiome Project

10. Human Microbiome Project

11. Human Microbiome Project
Different body sites have their own distinctive communities
Microbes colonize each site to use available sugars
Variations in the enzymes for carbohydrate metabolism from site to site
Carbohydrate metabolites may be the most important factor shaping the composition of microbial sub-communities of the human microbiome

12. Human Microbiome Project
Mouth and the gut have greater diversity of organisms than the skin and vagina
Bacterial makeup for a given body site varies from person to person by type and abundance
Bacteria of the same species composed of multiple subtypes

13. Human Microbiome Project
The vast majority of bacteria live in the large intestine
Archaea
Bacteria
Fungi
Mutualistic, symbiotic relationship
Fermentation for energy
Digestion
Train our immune system
Produce vitamins such as Vitamin K
Produce hormones to help store fat

15. Decreased Diversity of the Fecal Microbiome in Recurrent Clostridial difficile (CDI) Associated Diarrhea
Diarrhea is a common side effect of the administration of antibiotics
CDI is associated with most of the severe cases of antibiotic-associated diarrhea (AAD)
Ingestion of environmental spores
Overgrowth of indigenous CDI
Standard treatment for CDI includes metronidazole or vancomycin
Treatment of recurrent CDI can be difficult and has led to dramatic interventions, such as the administration of donor stool from healthy volunteers

16. Decreased Diversity of the Fecal Microbiome in Recurrent CDI Associated Diarrhea
The mechanisms by which antibiotics lead to CDI are not entirely clear
16S rRNA sequences amplified by PCR to profile the community structure of the gut microbiota of patients with initial CDI and recurrent CDI
Sequences grouped into operational taxonomic units (OTUs)
Ecological diversity measures calculated using the Shannon Index
Chang JY, Antonopoulos DA, Kalra A, et al. JID 2008:

17. Decreased Diversity of the Fecal Microbiome in Recurrent CDI Associated Diarrhea
3 control subjects and 7 patients with CDI
Microbial communities in each subject were compared and characterized at the phylum level
3 control subjects and the 4 patients with initial CDI
Bacteroides and Firmicutes
3 patients with recurrent CDI
More variable microbiota and lack of predominance of Bacteroides and Firmicutes
Chang JY, Antonopoulos DA, Kalra A, et al. JID 2008:

18. Decreased Diversity of the Fecal Microbiome in Recurrent CDI Associated Diarrhea
Chang JY, Antonopoulos DA, Kalra A, et al. JID 2008:

19. Chang JY, Antonopoulos DA, Kalra A, et al. JID 2008:197 435 -438

20. Conclusions
Changes in the gut microbiome have been associated with obesity, inflammatory bowel disease and AAD
Changes in metabolic activity of the altered microbial community
Changes in the interaction between the microbiome and the host immune system
“Colonization Resistance” of indigenous gut microbiota
Breakdown in colonization resistance
Suppression of indigenous microbiota
Expansion of pre-existing CDI or germination and expansion of CDI spores acquired from the environment
Chang JY, Antonopoulos DA, Kalra A, et al. JID 2008:

21. Conclusions Standard treatment with metronidazole or vancomycin
Suppress CDI and allow recovery of indigenous microbiota with restoration of colonization resistance
Assumption: remaining microbiome is sufficiently diverse to recover to a “normal” state
Recurrent CDI
Recrudescence of the original strain or acquisition of a new strain
Assumption: remaining microbiome is deficient in the ability to restore colonization resistance
Chang JY, Antonopoulos DA, Kalra A, et al. JID 2008:

22. Treatment Options European Society of Clinical Microbiology and Infections
For nonepidemic, nonsevere CDI clearly induced by antibiotic use, with no signs of severe colitis, it may be acceptable to stop the inducing antibiotic and observe the clinical response for 48 hours.
Patients must be monitored very closely and treated immediately for any signs of clinical deterioration.

23. Treatment Options European Society of Clinical Microbiology and Infections
Antibiotic treatment is recommended for all cases of CDI except for very mild CDI, which is actually triggered by antibiotic use.
Suitable antibiotics include metronidazole, vancomycin, and fidaxomicin
For mild/moderate disease, metronidazole is recommended as oral antibiotic treatment of initial CDI (500 mg 3 times daily for 10 days)
Fidaxomicin may be used in all CDI patients for whom oral antibiotic treatment is appropriate. Specific indications for fidaxomicin may include first-line treatment in patients with first CDI recurrence or at risk for recurrent disease, in patients with multiple recurrences of CDI, and in patients with severe disease and nonsevere CDI.

24. Treatment Options European Society of Clinical Microbiology and Infections
Recommendations based on two large phase 3 clinical studies
400 mg/day oral fidaxomicin vs 500 mg/day oral vancomycin
the rate of CDI recurrence was lower with fidaxomicin, but the cure rate was similar for both treatments
February 3, 2011Louie T.J., Miller M.A., Mullane K.M., et al.
N Engl J Med 2011; 364:

25. Treatment Options European Society of Clinical Microbiology and Infections
For severe CDI
vancomycin 125 mg 4 times daily (may be increased to 500 mg 4 times daily) for 10 days
fidaxomicin 200 mg twice daily for 10 days.
In life-threatening CDI, there is no evidence supporting the use of fidaxomicin
In severe CDI or life-threatening disease, the use of oral metronidazole is strongly discouraged

26. Annals of Surgery Volume 254, Number 3, September 2011
Treatment Options European Society of Clinical Microbiology and Infections
For multiple recurrent CDI, fecal transplantation is strongly recommended
Total abdominal colectomy or diverting loop ileostomy combined with colonic lavage is recommended for CDI with colonic perforation and/or systemic inflammation and deteriorating clinical condition despite antibiotic treatment
Annals of Surgery Volume 254, Number 3, September 2011
Additional measures for CDI management include discontinuing unnecessary antimicrobial therapy, adequate fluid and electrolyte replacement, avoiding antimotility medications, and reviewing proton pump inhibitor use

27. Fecal Transplantation
Amsterdam
Adults with CDI relapse
Not immunosuppressed
Not on pressors
Not in ICU
Not pregnant
January 31, 2013
van Nood E., Vrieze A., Nieuwdorp M., et al.
N Engl J Med 2013; 368:

28. Fecal Transplantation
Donors
< 60 years of age
Screened for a variety of transimissable diseases
Sample collected on the day of infusion
500 ml of saline
Infused via NGT
50 ml over 3 minutes
January 31, 2013
van Nood E., Vrieze A., Nieuwdorp M., et al.
N Engl J Med 2013; 368:

29. Fecal Transplantation
January 31, 2013
van Nood E., Vrieze A., Nieuwdorp M., et al.
N Engl J Med 2013; 368:

30. Fecal Transplantation
January 31, 2013
van Nood E., Vrieze A., Nieuwdorp M., et al.
N Engl J Med 2013; 368:

31. Fecal Transplantation
January 31, 2013
van Nood E., Vrieze A., Nieuwdorp M., et al.
N Engl J Med 2013; 368:

32. Fecal Transplantation
January 31, 2013
van Nood E., Vrieze A., Nieuwdorp M., et al.
N Engl J Med 2013; 368:

33. Fecal Transplantation
January 31, 2013
van Nood E., Vrieze A., Nieuwdorp M., et al.
N Engl J Med 2013; 368:

34. Fecal Transplantation
Bacteriotherapy
16sRNA sequencing before and after fecal transplant
Prior to therapy
Deficient in Bacteroides and Firmicutes
14 days post transplant
Fecal composition of the recipient highly similar to the donor
Dominated by Bacteroides
Resolution of symptoms
Khoruts A, Dicksyed J, Jansson JK, Sadowsky MJ. J Clin Gastroenterol
2010 May – Jun; 44(5);

35. ID Week 2013 Fecal Transplantation
University of Calgary
Pills
Centrifuge
Encapsulate in three layers of gelatin
Release in colon
24 – 34 capsules
27 patients
100% with resolution
40 patients
98% with resolution
ID Week Abstract 89. Presented October 3, 2013

36. ID Week 2013 Fecal Transplantation
University of Calgary
Patient Satisfaction
9.6 overall
9.9 for ease
9.9 would recommend
ID Week Abstract 89. Presented October 3, 2013

37. Fecal Transplantation
“It's the yuck factor that has to be overcome, and it's the physicians, not the patients.”
Dr. Tom Moore
University of Kansas School of Medicine
ID Week Abstract 89. Presented October 3, 2013

38. Cost-effectiveness for Management of Recurrent CDI
Decision analytic model
Metronidazole
Vancomycin
Fidaxomycin
Fecal microbiota transplant (FMT)
FMT
Colonoscopy
Duodenal infusion
Enema
Konijeti GG, Sauk J, Shrime MG, et al. March 31, 2014: 1 - 6

39. Cost-effectiveness for Management of Recurrent CDI
Cohorts of patients with a median age of 65 years
1 year follow-up
PCR testing for CDI
Heterogeneous patient population of 027 and non-027 strains
Healthy
Mild-moderate CDI
Severe CDI
Persistent recurrent disease
Postcolectomy
Death
Konijeti GG, Sauk J, Shrime MG, et al. March 31, 2014: 1 - 6

40. Cost-effectiveness for Management of Recurrent CDI
Treatment algorithms consistent with previously presented guidelines
Median hospital duration of two weeks
FMT colonoscopy was the most cost-effective strategy for recurrent CDI
Cure rates > 88%
Recurrence rates < 15%
$2,724
Vancomycin preferred in settings where FMT not available
Konijeti GG, Sauk J, Shrime MG, et al. March 31, 2014: 1 - 6

41. It may end with the microbiome
but it begins with antibiotics and stewardship
Chang JY, Antonopoulos DA, Kalra A, et al. JID 2008:

42. Thank You