Cyclosporiasis · Cyclospora is different from bacterial foodborne pathogens Bacteria are haploid...
Transcript of Cyclosporiasis · Cyclospora is different from bacterial foodborne pathogens Bacteria are haploid...
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Center for Global Health
Cyclosporiasis
Anne Straily, DVM, MPH, DACVPM Veterinary Medical Officer, Parasitic Diseases Branch, Division of Parasitic Diseases and Malaria
Centers for Disease Control and Prevention
Rocky Mountain Food Safety Conference
May 9, 2018
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Cyclospora cayetanensis
Coccidian protozoan parasite
Humans are only known reservoir
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Life cycle
Unsporulated oocysts shed in stool
– Require some time in favorable environmental conditions to sporulate (become infectious)
Sporulated oocysts contaminate produce and/or water sources
Oocysts do not multiply outside of human host
No direct person-to-person transmission
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Cyclosporiasis
Endemic in subtropical and tropical regions
U.S. infections typically are associated with either:
– International travel to areas of endemicity
– Consumption of imported fresh produce from areas of endemicity
Infections in persons with domestically-acquired illness (i.e. no history of international travel in the 2 weeks preceding illness onset) tend to be seasonal with peaks during May to August
– It is unknown what environmental conditions drive this seasonality
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Clinical Illness
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Clinical illness – symptoms
Incubation period ~ 1 week (range: 2 to 14 days)
Symptoms
– Watery diarrhea (most common)
– Loss of appetite
– Weight loss
– Cramping
– Bloating
– Increased gas
– Nausea
– Fatigue
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Clinical illness
Often follows remitting-relapsing course
If untreated, symptoms can last for days to weeks to months
Substantial weight loss and fatigue can occur in prolonged illness
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Diagnosing cyclosporiasis
2 methods are available:
– Ova and Parasite examination (O&P)
– Multi-pathogen molecular testing panels
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Diagnostic methods: Ova & Parasite examination (O&P)
Stools examined by routine O&P do not usually include Cyclospora
– Physician must specifically request Cyclospora testing
Requires special techniques and training
– UV fluorescence microscopy (oocysts are autofluorescent)
– Acid fast staining
Oocysts blend in with the background on unstained
slides
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Detection of Cyclospora oocysts by microscopy
Acid fast staining of oocysts (note that not all oocysts retain the stain)
UV fluorescence microscopy
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Diagnostic methods: Multi-pathogen molecular testing panels
A single stool specimen tested via polymerase chain reaction (PCR) for multiple pathogens simultaneously
Cyclospora included only in one commercially-available panel
– Became available in 2014
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Diagnosis can be difficult…
Even persons with profuse diarrhea might not shed enough oocysts to be readily detectable
– Requires use of sensitive recovery and detection methods
Parasite shed intermittently
– May require multiple stool specimens from different days
If testing is done by O&P, the physician must specifically request testing for Cyclospora
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Diagnostic methods: What’s not available
Many common tools available for diagnosing other foodborne pathogens are not available for Cyclospora
– Culture
– Whole-genome sequencing (WGS)
– Pulsed-field gel electrophoresis (PFGE)
– Molecular tools for strain differentiation
– Serologic assays
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Treatment of cyclosporiasis
Treatment of choice is trimethoprim-sulfamethoxazole (TMP/SMX)*
No highly effective alternatives have been identified for persons who are allergic or cannot tolerate TMP/SMX
TMP/SMX is different from medications commonly used for other enteric protozoan or bacterial infections
– Highlights importance of diagnosing infection rather than treating empirically
* Treatment of cyclosporiasis is not an FDA-approved indication, thus this is an “off label use”
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Surveillance – Outbreak Detection & Monitoring
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U.S. surveillance for cyclosporiasis
Nationally notifiable since 1999
Currently reportable in 43 states, the District of Columbia, and New York City
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Case-patient diagnosed by
HCP
Reported to Local/State
Health Department
Case-patient interviewed by LHD/SHD
Data transmitted
to CDC
CDC compiles national level
data
U.S. surveillance for cyclosporiasis
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Previous outbreaks of cyclosporiasis
Foodborne outbreaks of cyclosporiasis have been reported in the U.S. since the mid-1990s
Linked to various types of imported fresh produce
– E.g., basil, cilantro, raspberries, snow peas, mesclun lettuce
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Previous outbreaks of cyclosporiasis
During 2000-2015, 32 foodborne outbreaks identified in the U.S.
– Total number of reported cases: 1,652
– Median of 2 outbreaks per year, with a median of 21 cases per outbreak (range: 3 to 582 cases)
– Food vehicle of infection identified for 14 of the 32 outbreaks (43%)
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2017 cyclosporiasis cases
A total of 1,151 laboratory-confirmed cases*
– 624 (54%) occurred in persons who did not report international travel and became ill on or after May 1, 2017
– Reported by 40 states and NYC
– Hospitalizations: 61
– Median onset date: 7/5/2017
– 56% female
– Median age: 47 years (range: 1–102 years)
– No deaths
*Data are preliminary and subject to change; current as of April 11, 2018
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Comparison of 2017 with previous years 2017* 2016 2015
Total number lab-confirmed cases**
1,151 522 604
Number of domestically-acquired cases with onset on/after May 1 (n, %)
624 (54%) 174 (33%) 331 (55%)
Reported by 40 states, DC, and NYC 38 states, DC, and NYC 34 states and NYC
% Female 56% 62% 56%
Median age (years) (Range)
47 years Range: 1—102 years
47 years Range: 1—99 years
46.5 years Range: 1—95 years
Median onset date July 5 July 8 June 23
Hospitalized (n, %) 61 (5%) 23 (4%) 29 (5%)
Deaths (n, %) 0 (0%) 0 (0%) 0 (0%)
*Data are preliminary and subject to change; current as of April 11, 2018; **There were a few cases reported from these years that were reported by states where cyclosporiasis is not explicitly reportable, therefore the totals may differ slightly from what is published in a surveillance summary
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Week of onset3
2016 2017
1Case-patients with no international travel history were included. Case-patients with pending, unknown, or missing travel history were not included. 2From completed case data received as of 4/11/18). 3Week of stool collection was used if onset date was missing (2016, n=2; 2017, n=11). If both onset date and stool collection date were missing, the case-patient was excluded (2016, n=2; 2017, n=9). If year of symptom onset was different than the year of report, the case-patient was excluded (2017, n=2). 4CDC typically sees an increase in reported cases during the months of May–August (weeks 22–35); these are the months that surveillance is typically enhanced by using the CNHGQ.
4See note
Reported cases of laboratory-confirmed, non-travel-associated1
cyclosporiasis, United States 2016 (n=200) and 2017 (n=659)2
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Laboratory-confirmed domestically acquired cases1 of cyclosporiasis with
onset on/after 1 May 2017 to present2 (n=624)
Most cases were reported from TX, FL, NC, and NY/NYC
Majority of cases have not been epidemiologically linked
1Case-patients indicated on map by state of residence. 2Includes cases reported to CDC for 2017 as of 4/11/2018, for which illness onset date is available.
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2017 cluster investigations
A cluster of cases was defined as 2 or more cases in persons who shared a common food/produce exposure
Clusters were identified in 10 states
Case-control studies initiated for 4 clusters in different states
– Only one identified a likely vehicle (green onions)
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Investigation Challenges
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Case-patient diagnosed by
HCP
Reported to Local/State
Health Department
Case-patient interviewed by LHD/SHD
Data transmitted
to CDC
CDC compiles national level
data
Anatomy of a cluster investigation
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Identify cluster
Investigate cluster
Implicate food
vehicle
Conduct traceback
investigation
Identify source
(e.g. farm)
Regulatory action
Anatomy of a cluster investigation
Case-patient diagnosed by
HCP
Reported to Local/State
Health Department
Case-patient interviewed by LHD/SHD
Data transmitted
to CDC
CDC compiles national level
data
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Identify cluster
Investigate cluster
Implicate food
vehicle
Conduct traceback
investigation
Identify source
(e.g. farm)
Regulatory action
Anatomy of a cluster investigation
2 or more cases with common food or produce exposure
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Identify cluster
Investigate cluster
Implicate food
vehicle
Conduct traceback
investigation
Identify source
(e.g. farm)
Regulatory action
Anatomy of a cluster investigation
• Restaurant/event-specific questionnaire
• Case control study
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Identify cluster
Investigate cluster
Implicate food
vehicle
Conduct traceback
investigation
Identify source
(e.g. farm)
Regulatory action
Anatomy of a cluster investigation
• Strength of association – e.g. attack rates, odds ratios
• Biological plausibility
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Identify cluster
Investigate cluster
Implicate food
vehicle
Conduct traceback
investigation
Identify source
(e.g. farm)
Regulatory action
Anatomy of a cluster investigation
State/Local Health
Department
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Identify cluster
Investigate cluster
Implicate food
vehicle
Conduct traceback
investigation
Identify source
(e.g. farm)
Regulatory action
Anatomy of a cluster investigation
State/Local Health
Department
Sometimes with assistance from
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Identify cluster
Investigate cluster
Implicate food
vehicle
Conduct traceback
investigation
Identify source
(e.g. farm)
Regulatory action
Anatomy of a cluster investigation
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Challenges in investigating cyclosporiasis clusters: Fresh produce vehicles
Typically consumed fresh and have a short shelf-life
Leftovers usually not available for testing by the time a vehicle of interest is identified
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Challenges in investigating cyclosporiasis clusters: Fresh produce vehicles
Fresh produce often served in mixtures and in inconspicuous ways (e.g. as garnishes)
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Challenges in investigating cyclosporiasis clusters: Case ascertainment
Making the diagnosis
– Routine O&P examinations do not typically include testing for Cyclospora
– Physician must specifically request testing
– Multi-pathogen panel tests: only one includes a target for Cyclospora, but others do not
Case reporting
– Physicians and laboratories need to report cases to local or state health departments
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Challenges in investigating cyclosporiasis clusters: Linking cases in place and time
No molecular subtyping tools have been validated for linking cases of cyclosporiasis to each other or to a particular vehicle or source
?
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Cyclospora is different from bacterial foodborne pathogens
Bacteria are haploid and reproduce asexually
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Cyclospora is different from bacterial foodborne pathogens
Bacteria are haploid and reproduce asexually
Haploid – having only one copy of a chromosome
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Cyclospora is different from bacterial foodborne pathogens
Bacteria are haploid and reproduce asexually
Haploid – having only one copy of a chromosome
Diploid – having two copies of each chromosome
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Cyclospora is different from bacterial foodborne pathogens
Bacteria are haploid and reproduce asexually
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Cyclospora is different from bacterial foodborne pathogens
Bacteria are haploid and reproduce asexually
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Cyclospora is different from bacterial foodborne pathogens
Bacteria are haploid and reproduce asexually
Each new daughter cell is essentially a genetically identical clone of the parent cell
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Cyclospora is different from bacterial foodborne pathogens
Bacteria are haploid and reproduce asexually
– Suitable for source-linkage analyses because the bacteria present in a case-patient would be genetically very similar to bacteria in source food
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Cyclospora is different from bacterial foodborne pathogens
Bacteria are haploid and reproduce asexually
– Suitable for source-linkage analyses because the bacteria present in a case-patient would be genetically very similar to bacteria in source food
Cyclospora are diploid organisms and reproduce both sexually and asexually
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Cyclospora is different from bacterial foodborne pathogens
Bacteria are haploid and reproduce asexually
– Suitable for source-linkage analyses because the bacteria present in a case-patient would be genetically very similar to bacteria in source food
Cyclospora are diploid organisms and reproduce both sexually and asexually
– Daughter cells are a genetic blend of the parent cells
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Cyclospora is different from bacterial foodborne pathogens
Bacteria are haploid and reproduce asexually
– Suitable for source-linkage analyses because the bacteria present in a case-patient would be genetically very similar to bacteria in source food
Cyclospora are diploid organisms and reproduce both sexually and asexually
– Daughter cells are a genetic blend of the parent cells
– After multiple generations there can be significant genetic divergence
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Cyclospora is different from bacterial foodborne pathogens
Unable to grow it in the laboratory
– No multiplication outside humans (only known amplifying hosts)
– No culture system or animal model
– Human volunteer studies have not been successful
No way to maintain isolates for study
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Challenges in investigating cyclosporiasis clusters: Linking cases in place and time
No molecular subtyping tools have been validated for linking cases of cyclosporiasis to each other or to a particular vehicle or source
Exposure histories are used to link cases epidemiologically
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Challenges in investigating cyclosporiasis clusters: Linking cases in place and time
No molecular subtyping tools have been validated for linking cases of cyclosporiasis to each other or to a particular vehicle or source
Exposure histories are used to link cases epidemiologically
– Case-patients may report multiple common exposures
– Identifying linkages among 500+ cases is difficult
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Challenges in investigating cyclosporiasis clusters: Linking cases in place and time
No molecular subtyping tools have been validated for linking cases of cyclosporiasis to each other or to a particular vehicle or source
Exposure histories are used to link cases epidemiologically
Interviewing case-patients can take a substantial amount of time
– CDC requests that states administer a hypothesis generating questionnaire to all case-patients with illness onset during May-August
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Challenges in investigating cyclosporiasis clusters: Linking cases in place and time
No molecular subtyping tools have been validated for linking cases of cyclosporiasis to each other or to a particular vehicle or source
Exposure histories are used to link cases epidemiologically
Interviewing case-patients can take a substantial amount of time
Case-control investigations
– Sub-optimal recall of food exposures
– Extensive menus, overlapping ingredients make identifying actual food vehicle or ingredient difficult
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Why are we seeing more cases and/or more outbreaks?
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Why Are we seeing more cases and/or more outbreaks?
Case numbers vary from year to year – what is “baseline”?
Did 2017 represent a true increase in case count?
– Each year, ~48 million people become ill from foodborne illness in U.S.
– Only ~20% of these have a specific pathogen identified
Are we diagnosing more of the cases that already existed?
– Increased provider awareness
– Readily available testing methods (multiplex pathogen panel)
– Improved testing methods
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Prevention & Control
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How does produce become contaminated?
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How does produce become contaminated?
Precise mechanism is not well understood
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Hypothetically, contamination may occur…
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Hypothetically, contamination may occur…
On the farm, if contaminated water sources are used to irrigate crops, or to mix and apply chemicals like herbicides or pesticides
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Hypothetically, contamination may occur…
On the farm, if contaminated water sources are used to irrigate crops, or to mix and apply chemicals like herbicides or pesticides
During processing, if contaminated water sources are used to rinse and wash produce
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Prevention and Control Personal measures
No vaccine is available
When traveling to areas endemic for Cyclospora
– Avoid food or water that may have been contaminated with feces
– “If you can’t cook it, peel it, or wash it – then forget it”
Follow safe fruit and vegetable handling recommendations
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Prevention and Control Restaurant owners and food handlers
Cyclospora does not multiply outside the human host
– No direct human-to-human transmission occurs
– Not an “ill food handler” issue
Fresh produce contaminated prior to arrival at establishment
– Not a restaurant sanitation issue
Time and temperature rules to prevent growth of bacterial pathogens not helpful in control of Cyclospora
Treatment with chlorine or iodine unlikely to kill oocysts at concentrations used for routine sanitization
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Prevention and Control Industry measures
FDA’s Center for Food Safety and Applied Nutrition publishes food safety recommendations for growers and suppliers
– These guidelines describe good agricultural practices and good manufacturing practices for fresh fruits and vegetables
– Following these guidelines can help reduce the overall risk for microbial contamination during growing, harvesting, sorting, packaging and storage
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What can be done about Cyclospora?
IF a food vehicle can be identified AND traced back to the source, then FDA can potentially take regulatory action
Examples
– Import ban on cilantro from Puebla, Mexico
– Import ban on fresh Guatemalan raspberries in late 1990s
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What is CDC doing?
Year-round surveillance with enhanced surveillance conducted during May through August/September
Educate healthcare providers about diagnosing Cyclospora
Provide timely epidemiological updates during cyclosporiasis season
Collaborate with state and local health departments to investigate cases and disseminate data
Provide outbreak/cluster investigation assistance when requested
Alert healthcare providers and health departments about outbreaks/clusters/increased cases when necessary
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What is CDC doing?
Develop molecular typing methods that can be used to link cases or implicate food vehicles and sources
– Cyclospora Advanced Molecular Detection initiative
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Acknowledgements
State and Local Health Departments
Food and Drug Administration
Centers for Disease Control and Prevention
– Division of Parasitic Diseases and Malaria
– Division of Foodborne, Waterborne, and Environmental Diseases
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For more information, contact CDC 1-800-CDC-INFO (232-4636) TTY: 1-888-232-6348 www.cdc.gov The findings and conclusions in this report are those of the authors and do not necessarily represent the official position of the Centers for Disease Control and Prevention.
Thank you for your attention! Questions?