Chains of Transmission and Control of Ebola Virus Disease in Conakry, Guinea, in 2014: an Observational Study

Overview

Journal Lancet Infect Dis

Specialty Infectious Diseases

Date 2015 Jan 27

PMID 25619149

Citations 119

Authors

Ousmane Faye

Pierre-Yves Boelle

Emmanuel Heleze

Oumar Faye

Cheikh Loucoubar

NFaly Magassouba

Barre Soropogui

Sakoba Keita

Tata Gakou

El Hadji Ibrahima Bah

Lamine Koivogui

Amadou Alpha Sall

Simon Cauchemez

Affiliations

Soon will be listed here.

Abstract

Background: An epidemic of Ebola virus disease of unprecedented size continues in parts of west Africa. For the first time, large urban centres such as Conakry, the capital of Guinea, are affected. We did an observational study of patients with Ebola virus disease in three regions of Guinea, including Conakry, aiming to map the routes of transmission and assess the effect of interventions.

Methods: Between Feb 10, 2014, and Aug 25, 2014, we obtained data from the linelist of all confirmed and probable cases in Guinea (as of Sept 16, 2014), a laboratory database of information about patients, and interviews with patients and their families and neighbours. With this information, we mapped chains of transmission, identified which setting infections most probably originated from (community, hospitals, or funerals), and computed the context-specific and overall reproduction numbers.

Findings: Of 193 confirmed and probable cases of Ebola virus disease reported in Conakry, Boffa, and Télimélé, 152 (79%) were positioned in chains of transmission. Health-care workers contributed little to transmission. In March, 2014, individuals with Ebola virus disease who were not health-care workers infected a mean of 2·3 people (95% CI 1·6-3·2): 1·4 (0·9-2·2) in the community, 0·4 (0·1-0·9) in hospitals, and 0·5 (0·2-1·0) at funerals. After the implementation of infection control in April, the reproduction number in hospitals and at funerals reduced to lower than 0·1. In the community, the reproduction number dropped by 50% for patients that were admitted to hospital, but remained unchanged for those that were not. In March, hospital transmissions constituted 35% (seven of 20) of all transmissions and funeral transmissions constituted 15% (three); but from April to the end of the study period, they constituted only 9% (11 of 128) and 4% (five), respectively. 82% (119 of 145) of transmission occurred in the community and 72% (105) between family members. Our simulations show that a 10% increase in hospital admissions could have reduced the length of chains by 26% (95% CI 4-45).

Interpretation: In Conakry, interventions had the potential to stop the epidemic, but reintroductions of the disease and poor cooperation of a few families led to prolonged low-level spread, showing the challenges of Ebola virus disease control in large urban centres. Monitoring of chains of transmission is crucial to assess and optimise local control strategies for Ebola virus disease.

Funding: Labex IBEID, Reacting, PREDEMICS, NIGMS MIDAS initiative, Institut Pasteur de Dakar.

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References

Whitty C, Farrar J, Ferguson N, Edmunds W, Piot P, Leach M . Infectious disease: tough choices to reduce Ebola transmission. Nature. 2014; 515(7526):192-4. DOI: 10.1038/515192a. View

Weidmann M, Muhlberger E, Hufert F . Rapid detection protocol for filoviruses. J Clin Virol. 2004; 30(1):94-9. DOI: 10.1016/j.jcv.2003.09.004. View

Jombart T, Cori A, Didelot X, Cauchemez S, Fraser C, Ferguson N . Bayesian reconstruction of disease outbreaks by combining epidemiologic and genomic data. PLoS Comput Biol. 2014; 10(1):e1003457. PMC: 3900386. DOI: 10.1371/journal.pcbi.1003457. View

Fasina F, Shittu A, Lazarus D, Tomori O, Simonsen L, Viboud C . Transmission dynamics and control of Ebola virus disease outbreak in Nigeria, July to September 2014. Euro Surveill. 2014; 19(40):20920. DOI: 10.2807/1560-7917.es2014.19.40.20920. View

Pandey A, Atkins K, Medlock J, Wenzel N, Townsend J, Childs J . Strategies for containing Ebola in West Africa. Science. 2014; 346(6212):991-5. PMC: 4316831. DOI: 10.1126/science.1260612. View

Aylward B, Barboza P, Bawo L, Bertherat E, Bilivogui P, Blake I . Ebola virus disease in West Africa--the first 9 months of the epidemic and forward projections. N Engl J Med. 2014; 371(16):1481-95. PMC: 4235004. DOI: 10.1056/NEJMoa1411100. View

Fraser C, Riley S, Anderson R, Ferguson N . Factors that make an infectious disease outbreak controllable. Proc Natl Acad Sci U S A. 2004; 101(16):6146-51. PMC: 395937. DOI: 10.1073/pnas.0307506101. View

Gomes M, Pastore Y Piontti A, Rossi L, Chao D, Longini I, Halloran M . Assessing the international spreading risk associated with the 2014 west african ebola outbreak. PLoS Curr. 2015; 6. PMC: 4169359. DOI: 10.1371/currents.outbreaks.cd818f63d40e24aef769dda7df9e0da5. View

Wesolowski A, Buckee C, Bengtsson L, Wetter E, Lu X, Tatem A . Commentary: containing the ebola outbreak - the potential and challenge of mobile network data. PLoS Curr. 2015; 6. PMC: 4205120. DOI: 10.1371/currents.outbreaks.0177e7fcf52217b8b634376e2f3efc5e. View

10.

Althaus C . Estimating the Reproduction Number of Ebola Virus (EBOV) During the 2014 Outbreak in West Africa. PLoS Curr. 2015; 6. PMC: 4169395. DOI: 10.1371/currents.outbreaks.91afb5e0f279e7f29e7056095255b288. View

11.

Fisman D, Khoo E, Tuite A . Early epidemic dynamics of the west african 2014 ebola outbreak: estimates derived with a simple two-parameter model. PLoS Curr. 2015; 6. PMC: 4169344. DOI: 10.1371/currents.outbreaks.89c0d3783f36958d96ebbae97348d571. View

12.

Ksiazek T, Rollin P, Williams A, Bressler D, Martin M, Swanepoel R . Clinical virology of Ebola hemorrhagic fever (EHF): virus, virus antigen, and IgG and IgM antibody findings among EHF patients in Kikwit, Democratic Republic of the Congo, 1995. J Infect Dis. 1999; 179 Suppl 1:S177-87. DOI: 10.1086/514321. View