Geotemporal analysis of Neisseria meningitidis clones in the United States: 2000-2005.

Ann E Wiringa Kathleen A Shutt Jane W Marsh Amanda C Cohn Nancy E Messonnier Shelley M Zansky Susan Petit Monica M Farley Ken Gershman Ruth Lynfield Arthur Reingold William Schaffner Jamie Thompson Shawn T Brown Bruce Y Lee Lee H Harrison

PLoS One

Infectious Diseases Epidemiology Research Unit, University of Pittsburgh Graduate School of Public Health and School of Medicine, Pittsburgh, Pennsylvania, United States of America ; Department of International Health, Johns Hopkins Bloomberg School of Public Health, Baltimore, Maryland, United States of America.

Published: September 2014

* From 2000 to 2005, 1,062 meningococcal cases were analyzed, revealing 438 unique clones, with 66% of cases linked to non-singleton clones and 32 significant clusters identified across various locations and time frames.
* The findings indicate that about 10% of cases are associated with specific geotemporal clusters, emphasizing the importance of molecular characterization and spatial analysis in understanding and preventing meningococcal outbreaks.

Background: The detection of meningococcal outbreaks relies on serogrouping and epidemiologic definitions. Advances in molecular epidemiology have improved the ability to distinguish unique Neisseria meningitidis strains, enabling the classification of isolates into clones. Around 98% of meningococcal cases in the United States are believed to be sporadic.

Methods: Meningococcal isolates from 9 Active Bacterial Core surveillance sites throughout the United States from 2000 through 2005 were classified according to serogroup, multilocus sequence typing, and outer membrane protein (porA, porB, and fetA) genotyping. Clones were defined as isolates that were indistinguishable according to this characterization. Case data were aggregated to the census tract level and all non-singleton clones were assessed for non-random spatial and temporal clustering using retrospective space-time analyses with a discrete Poisson probability model.

Results: Among 1,062 geocoded cases with available isolates, 438 unique clones were identified, 78 of which had ≥2 isolates. 702 cases were attributable to non-singleton clones, accounting for 66.0% of all geocoded cases. 32 statistically significant clusters comprised of 107 cases (10.1% of all geocoded cases) were identified. Clusters had the following attributes: included 2 to 11 cases; 1 day to 33 months duration; radius of 0 to 61.7 km; and attack rate of 0.7 to 57.8 cases per 100,000 population. Serogroups represented among the clusters were: B (n = 12 clusters, 45 cases), C (n = 11 clusters, 27 cases), and Y (n = 9 clusters, 35 cases); 20 clusters (62.5%) were caused by serogroups represented in meningococcal vaccines that are commercially available in the United States.

Conclusions: Around 10% of meningococcal disease cases in the U.S. could be assigned to a geotemporal cluster. Molecular characterization of isolates, combined with geotemporal analysis, is a useful tool for understanding the spread of virulent meningococcal clones and patterns of transmission in populations.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3861328	PMC
http://journals.plos.org/plosone/article?id=10.1371/journal.pone.0082048	PLOS

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