Publications by authors named "Michael H Woodworth"

Microbiota-based therapies are used increasingly for the treatment and prevention of Clostridioides difficile infection (CDI), particularly in cases of recurrent CDI (rCDI). This review discusses the different types of microbiota-based therapies, including fecal microbiota transplant, fecal microbiota products, and live biotherapeutic products. The authors present efficacy data regarding clinical use in rCDI and highlight the unique aspects of each product.

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More than 850 million individuals worldwide, accounting for 10-15% of the adult population, are estimated to have chronic kidney disease. Each of these individuals is host to tens of trillions of microorganisms that are collectively referred to as microbiota - a dynamic ecosystem that both influences host health and is itself influenced by changes in the host. Available evidence supports the existence of functional connections between resident microorganisms and kidney health that are altered in the context of specific kidney diseases, including acute kidney injury, chronic kidney disease and renal stone disease.

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Importance: Intestinal multidrug-resistant organism (MDRO) colonization is highly prevalent in long-term acute care hospital (LTACH) patients and is associated with MDRO infection and transmission. However, there are no therapies approved by the US Food and Drug Administration to reduce intestinal MDRO colonization.

Objective: To determine the safety and acceptability of fecal microbiota transplantation (FMT) in LTACH patients.

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While the inhibitory receptor FcγRIIB has been shown to be upregulated on activated CD8+ T cells in both mice and humans, its effect on T cell fate during infection has not been fully elucidated. We identified an increase in FcγRIIB-expressing CD8+ T cells in patients with COVID-19 relative to healthy controls as well as in mouse models of viral infection. Despite its well-known role as an Fc receptor, FcγRIIB also ligates the immunosuppressive cytokine Fgl2, resulting in CD8+ T cell apoptosis.

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The enteric microbiota is an established reservoir for multidrug-resistant organisms that present urgent clinical and public health threats. Observational data and small interventional studies suggest that microbiome interventions, such as fecal microbiota products and characterized live biotherapeutic bacterial strains, could be an effective antibiotic-sparing prevention approach to address these threats. However, bacterial colonization is a complex ecological phenomenon that remains understudied in the context of the human gut.

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With the increase in the placement of prosthetic joints and other hardware in the body has come an increase in associated infections. These infections are particularly difficult to treat due to the underlying bacteria generating matrices which resist clearance by immune system effectors or antibiotics. These matrices, biofilms, have two primary ways of being eradicated, either by physical removal by debridement or by killing the underlying bacteria.

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Introduction: Maribavir was recently approved by the FDA, expanding treatment options for post-solid-organ transplant refractory/resistant CMV. We sought to describe the post-marketing experience with maribavir at a large academic transplant center.

Methods: This was a retrospective observational study of all renal transplant recipients treated with maribavir for refractory/resistant CMV DNAemia/disease.

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Article Synopsis
  • Doxycycline post-exposure prophylaxis (doxy-PEP) is effective in reducing bacterial sexually transmitted infections among men who have sex with men and transgender women but raises concerns about its impact on antimicrobial resistance.
  • A study involving participants from the DoxyPEP trial assessed the effects of doxy-PEP on the gut microbiome and antimicrobial resistance genes by comparing metagenomic and metatranscriptomic data over six months between those receiving doxy-PEP and standard care.
  • Results showed an increase in tetracycline resistance genes among participants using doxy-PEP, with a significant enrichment of these genes correlated with the number of doxycycline doses taken.
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The gut, urine, and vaginal microbiomes play significant roles in the pathogenesis of recurrent urinary tract infections (rUTIs). Analysis of these microbiota has shown distinct associations with urinary tract infections. Encouraging data indicate that rUTIs may be responsive to microbiome treatments such as fecal microbiota transplantation, expanding potential treatments beyond antibiotics, hydration, and behavioral interventions.

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Article Synopsis
  • * A case of a 60-year-old woman is presented who developed E. rhusiopathiae bacteremia after injuring her leg in a sewer, with no clear animal contact, suggesting sewage as the source.
  • * She improved after being treated with intravenous penicillin, but due to her circumstances, she was switched to an oral antibiotic, linezolid, which was successful, highlighting the bacteria's resistance to vancomycin and limited alternatives for treatment.
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Food and Drug Administration approval of the first microbiome therapies represents a true expansion the treatment paradigm for Clostridioides difficile but raises new questions about the future role of fecal microbiota transplantation. The authors outline the advances in microbiome therapeutic development that have addressed fecal microbiota transplantation's (FMT's) inherent limitations of safety and scalability. The authors also suggest that as microbiome therapeutic development continues for other indications, FMT will likely remain a necessary model of human microbiota dynamics for translational research.

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Background: Fecal microbiota transplantation (FMT) is recommended for the treatment of recurrent infection (rCDI). In the current study, we evaluated rates of rCDI and subsequent FMT in a large metropolitan area. We compared demographic and clinical differences in FMT recipients and nonrecipients and quantified differences in outcomes based on treatment modality.

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Article Synopsis
  • A study investigated the impact of multidrug-resistant organisms (MDRO) and similar antibiotic-susceptible organisms (CSO) on kidney transplant patients in the early post-transplant period (within 30 days of surgery).
  • Out of 3507 renal transplant recipients (RTRs), only 1.3% showed MDRO detection, but this was linked to significantly higher risks of both graft loss and mortality.
  • The findings suggest that routine screening and preventive measures for MDROs could improve outcomes for kidney transplant patients.
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  • CMV infections pose significant health risks for solid organ transplant recipients, leading to increased morbidity and mortality rates.
  • Traditional prevention methods include prophylactic, preemptive, and hybrid strategies, but new research emphasizes the potential of using CMV-specific immune assays for personalized risk assessment.
  • The effectiveness of these assays can vary based on timing related to the transplant and the type of immunosuppressive treatment, with a focus on measuring CD4+ and CD8+ T-Cell responses for a comprehensive understanding of immune recovery.
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Background: Cytomegalovirus (CMV) infection has broad implications for morbidity and mortality in renal transplant recipients (RTR). Routine surveillance for CMV replication with PCR-based quantitative nucleic acid testing (qNAT) assays is standard practice in most transplant centers, but the impact of assay sensitivity on antiviral decision-making and virologic outcomes has not been studied. We investigated the effects of an ultrasensitive CMV qNAT assay on multiple clinical outcomes, including time to detection and duration of CMV DNAemia.

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There is a surfeit of bioinformatic data showing that bacteriophages abound in the enteric microbiomes of humans. What is the contribution of these viruses in shaping the bacterial strain and species composition of the gut microbiome and how are these phages maintained over time? To address these questions, we performed experiments with and phages isolated from four fecal microbiota transplantation (FMT) doses as representative samples of non-dysbiotic enteric microbiota and develop and analyze the properties of a mathematical model of the population and evolutionary dynamics of bacteria and phage. Our models predict and experiments confirm that due to production of the O antigen, in the enteric microbiome are likely to be resistant to infection with co-occurring phages.

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Multidrug-resistant organism (MDRO) colonization is a fundamental challenge in antimicrobial resistance. Limited studies have shown that fecal microbiota transplantation (FMT) can reduce MDRO colonization, but its mechanisms are poorly understood. We conducted a randomized, controlled trial of FMT for MDRO decolonization in renal transplant recipients called PREMIX (NCT02922816).

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Colistin is a last-resort antibiotic for multidrug-resistant Gram-negative infections. Recently, the ninth allele of the mobile colistin resistance () gene family, designated was reported. However, its clinical and public health significance remains unclear.

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Article Synopsis
  • * A case study revealed a patient with fever, abdominal pain, and enlarged liver, who was diagnosed with both bacillary peliosis hepatis and secondary haemophagocytic lymphohistiocytosis, after exposure to a sick dog.
  • * The patient was successfully treated with doxycycline and adjustments to immunosuppressive medication, highlighting the need for awareness of Bartonella infections in cases of unexplained hemophagocytic lymphohistiocytosis, especially in patients with related symptoms and animal exposure.
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Obesity and obesity-related metabolic disorders are linked to the intestinal microbiome. However, the causality of changes in the microbiome-host interaction affecting energy metabolism remains controversial. Here, we show the microbiome-derived metabolite δ-valerobetaine (VB) is a diet-dependent obesogen that is increased with phenotypic obesity and is correlated with visceral adipose tissue mass in humans.

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Advances in genomics have revealed many of the genetic underpinnings of human disease, but exposomics methods are currently inadequate to obtain a similar level of understanding of environmental contributions to human disease. Exposomics methods are limited by low abundance of xenobiotic metabolites and lack of authentic standards, which precludes identification using solely mass spectrometry-based criteria. Here, we develop and validate a method for enzymatic generation of xenobiotic metabolites for use with high-resolution mass spectrometry (HRMS) for chemical identification.

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In this review, we discuss stool donor screening considerations to mitigate potential risks of pathogen transmission through fecal microbiota transplant (FMT) in solid organ transplant (SOT) recipients. SOT recipients have a higher risk for Clostridioides difficile infection (CDI) and are more likely to have severe CDI. FMT has been shown to be a valuable tool in the treatment of recurrent CDI (RCDI); however, guidelines for screening for opportunistic infections transmitted through FMT are underdeveloped.

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