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Table 2 Multivariable analysis of epidemiologic exposures and intestinal bacterial taxa related to Clostridium difficile infection (CDI) development

From: Reductions in intestinal Clostridiales precede the development of nosocomial Clostridium difficile infection

Variable

Phylum-level analysis

 

V1-V3 sequence set

V3-V5 sequence set

 

P valuea

Coefficient signb

P valuea

Coefficient signb

Bacterial phylum

  Bacteroidetes

0.048

-

0.061

-

Shannon diversity

0.187

-

0.455

-

Medication usec

  H2 blocker

0.319

-

0.271

-

  Nonsteroidal anti-inflammatory drug

0.684

+

0.989

+

  Proton-pump inhibitor

0.443

-

0.467

-

  Cephalosporin

0.016

+

0.009

+

  Fluoroquinolone

0.038

+

0.018

+

  Penicillin with β-lactamase inhibitor

0.228

+

0.424

+

  Vancomycind

0.278

+

0.116

+

 

Family-level analysis

 

V1-V3 sequence set

V3-V5 sequence set

 

P value a

Coefficient sign b

P value a

Coefficient sign b

Bacterial family

  Bacteroidaceae

0.073

-

0.051

-

  Clostridiales Incertae Sedis XI

0.015

-

0.025

-

  Enterococcaceae

0.942

+

0.246

+

Shannon diversity

0.728

+

0.238

+

Medication usec

  H2 blocker

0.384

-

0.318

-

  Nonsteroidal anti-inflammatory drug

0.921

+

0.605

+

  Proton-pump inhibitor

0.674

-

0.558

-

  Cephalosporin

0.020

+

0.027

+

  Fluoroquinolone

0.045

+

0.061

+

  Penicillin with β-lactamase inhibitor

0.692

+

0.850

-

  Vancomycind

0.423

+

0.193

+

  1. aP values were determined by multivariate logistic regression. bA positive sign indicates that 16S sequence abundance (for bacterial taxa) or number of patients exposed (for medications) was higher among patients with CDI than among controls, while a negative sign indicates that 16S sequence abundance or number of patients exposed was lower among patients with CDI. cDefined as use within 8 weeks before or during hospitalization, until stool collection. dIntravenous administration.
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Microbiome

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