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Analysis of Warning Process: Swine-Origin Triple Reassortant Influenza A(H3N2) Virus In USA

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by James Wilson, M.D. - Biosurveillance - December 21, 2011

We have been monitoring the situation with swine-origin triple reassortant influenza A(H3N2) virus (S-OtrH3N2) inside the United State for some time now.  Recent reports of likely human-human transmission sparked debate, discussed here in this post.

1.  First, the ECDC's risk assessment was an excellent discussion of the situation.  CDC's report may be found here.

2.  The time delays in issuing statements about the evolving situation reflect the forensic process and length of time it takes to recognize novel pathogens and execute public warning inside the United States.  In this case, a joint press releaseon Sept 2nd and 5th, respectively, from CDC and Pennsylvannia state officials announced recognition of S-OtrH3N2 pediatric cases in Indiana and Pennsylvania stemming from exposure to infected swine.  The breakdown of timelines as follows:

Case A (Indiana):

  • Day 0 (July 23rd).  Parental recognition of a child with flu-like illness.  Child brought to local ED, clinical laboratory testing at the hospital positive for type A influenza.   Child found to have been vaccinated the prior fall, had chronic medical condition, discharged from the ED same day without anti-virals.
  • Day 1 (July 24th).  Child returns to ED with a worsened clinical picture and admitted.
  • Day 4 (July 27th).  Child does well and is discharged from the inpatient ward to home.  No further issues.
  • Day 25 (Aug 17th).  Indiana State Department of Health Laboratories test the sample and discover suspect swine-origin influenza A (H3N2) virus.  CDC notified and sample forwarded to CDC for confirmation and further analysis.
  • Day 27 (Aug 19th).  CDC confirms findings of the Indiana State DOH Lab. 
  • Day 41 (Sep 2nd).  CDC reports publicly results of genomic sequencing: swine-origin triple reassortant influenza A(H3N2) virus that now includes segments of 2009 pandemic H1N1 virus.  Report indicates patient had contact with infected swine.
  • Summary:
    • Time delta: state public health recognition of unusual influenza virus= 25 days
    • Time delta: clinical processing of patient to CDC awareness= 25 days
    • Time delta: CDC issuance of warning to the public= 41 and 14 days from initial clinical processing of the patient and state notification to CDC, respectively

Case B (Pennsylvania):

  • Day 0 (Aug 20th).  Parental recognition of symptoms, take child to local ED.  Nasal swab positive for influenza A.  Child was vaccinated the prior fall.
  • Day 3 (Aug 23rd).  Pennsylvania State Department of Health Laboratory idenifies suspected swine-origin influenza A (H3N2) virus.
  • Day 4 (Aug 24th).  Pennsylvania state officials notify CDC of the findings.
  • Day 6 (Aug 26th).  CDC confirms findings.
  • Day 13 (Sep 2nd).  CDC reports publicly results of genomic sequencing: swine-origin triple reassortant influenza A(H3N2) virus that now includes segments of 2009 pandemic H1N1 virus.  Report indicates patient had contact with infected swine.
  • Summary:
    • Time delta: state public health recognition of unusual influenza virus= 3 days
    • Time delta: clinical processing of patient to CDC awareness= 4 days
    • Time delta: CDC issuance of warning to the public= 13 and 7 days from initial clinical processing of the patient and state notification to CDC, respectively

Questions were asked openly of CDC, USDA, and Pennsylvania state officials on Sept 12th about how these cases were recognized.  More to the point, guidance for clinical sampling was requested publicly.  This request was never answered.  At this point, the situation had migrated to the top of biological threat monitoring list.  Lack of response was not reassuring.

On Nov 23rd, a probable human-human transmission cluster of S-OtrH3N2 cases was reported by CDC, with an evident 7-10 day lag between initial clinical processing, laboratory based recognition at the state level, and CDC issuance of a public statement.  This was a much better time delta and likely reflective of surveillance grid sensitization this particular issue. 

Overall, we see a drop from a time delta between clinical processing and CDC issuance of public warning of these events from 41 to 13 to 7 days as the situation evolved.  It was not until Nov 26th did media reports indicate a seed strain had been sent to vaccine manufacturers in case S-OtrH3N2 begins to overtake current circulating strains of influenza virus in the human population.

There are several summary observations to make at this point:

  1. S-OtrH3N2 is our #1 pathogen of concern for the United States and the world at this time, from the perspective of potential social disruption.  Projected impact would be similar to that seen in a vaccine drift year of seasonal influenza (e.g. 2004 in the United States).  Thus far no fatalities have been observed, but the sample size is far too small at this time to make firm assertions of case fatality rate or morbidity profiles. 
  2. CDC should be praised for proactively forwarding seed stock to vaccine manufacturers.  What will be interesting to observe at this point is the time delta between initial recognition of sustained human-human transmission and an order to ramp up and distribute S-OtrH3N2 vaccine to local healthcare providers.  In this instance CDC stands in much better position to execute more efficient warning to response operational coupling.
  3. The above said, we note with great concern how long it took to recognize and effectively communicate to the public the initial situation in Indiana.  From the perspective of this author, a pediatrician practicing in a rural setting, there is no healthcare provider sensitization to this issue- i.e. there is no change at all in sampling procedures for children presenting with influenza-like illness.  It is as though this season is like any other.  Especially after the 2009 H1N1 pandemic experience and the current economic recession, we observe a general reluctance to test for influenza unless there is a compelling reason to do so.
  4. Not all states have the surveillance capabilities of Pennsylvania and Iowa.  There is an incomplete understanding of how pervasive S-OtrH3N2 transmission is inside the United States at this time. 
  5. Abrupt community inundation of pediatric flu-like illness, especially among children previously vaccinated for the 2010-2011 influenza season, should prompt an index of suspicion at least to obtain samples for testing by clinicians.  Submission of samples that are processed by state laboratories and moved up the chain to CDC is the only way to assess this evolving situation accurately.

http://biosurveillance.typepad.com/biosurveillance/2011/12/analysis-of-warning-process-swine-origin-triple-reassortant-influenza-ah3n2-virus-in-usa.html

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by James Wilson, M.D. - Biosurveillance - December 25, 2011

More Evidence of Human-Human Transmission of Swine-Origin Triple Reassortant Influenza A(H3N2) Virus In The United States

On December 23rd, CDC released another statement about the evolving situation with swine-origin triple reassortant influenza A(H3N2) virus in the United States.  Three more human infections, two of which associated with a daycare in West Virginia.  The latter is of greater concern than the former due to probable human-human transmission.  Time delays between submission of samples and public report by CDC remain high:

(Case A) Indiana, no evidence of human-human transmission- exposure from swine. 

  • Day 0 (Oct 20th).  Patient symptomatic, hospitalized for 4 days.
  • Day 2 (Oct 22nd).  Influenza-positive per in-house hospital laboratory testing.
  • Day 8 (Oct 28th).  Indiana State Public Health Laboratory: "inconclusive influenza A virus".
  • Day 11 (Oct 31st).  CDC confirms via genomic sequencing presence of "A(H3N2)v" (formerly known as S-OtrH3N2)
  • Day 64 (Dec 23rd).  CDC publicly releases the above information.
  • Summary:
    • Time delta: state public health recognition of unusual virus= 8 days
    • Time delta: clinical processing of patient to CDC awareness= 11 days
    • Time delta: CDC issuance of warning to the public= 64 and 56 days from initial clinical processing of the patient and state notification to CDC, respectively

(Cases B) West Virgina, evidence of human-human transmission.

  • Day 0 (Nov 12th, approximate).  Pediatric patient recognized symptomatic by parents.
  • Day 7 (Nov 19th).  Patient, who was already hospitalized for an unrelated issue, develops fever.
  • Day 9 (Nov 21st).  Sample taken.  In-house hospital laboratory discovers sample is positive for influenza A.  Patient discharged home.
  • ... No further information regarding when West Virginia's state laboratory or CDC processed the sample, which was A(H3N2)v-positive.
  • Summary:
    • Time delta: state public health recognition of unusual virus= unknown
    • Time delta: clinical processing of patient to CDC awareness= unknown
    • Time delta: CDC issuance of warning to the public= 34 days from initial clinical processing of the patient (approx. Nov 19th) 

(Case C) West Virginia, same cluster / thread.

  • Day 0 (Nov 29th).  2nd child at daycare center ill.
  • Day 9 (Dec 7th).  West Virginia Office of Laboratory Services processes sample as "inconclusive"- forwards on to CDC.  This patient was part of a retrospective assessment, where clinical processing did not occur.
  • .. No further information regarding when CDC processed the sample, which was A(H3N2)v-positive.
  • Summary:
    • Time delta: CDC issuance of warning to the public= 34 days from state public health laboratory processing of the sample to CDC issuance of public warning

 

The key point is of course, we only know what we are able to know.  Our team leaned into the discussion in November to ensure CDC was aware we were 1) monitoring the situation and 2) are carefully documenting their performance in coupling warning to response.  And quietly behind the scenes we are engaging clinical practitioners in an effort to encourage more sampling among symptomatic patients who were vaccinated for this season.  We expect the predominance of this focus to be on pediatric patients, however we are not seeing social sensitization yet among pediatricians.  Messaging from CDC requires clarification and guidance regarding when to sample.

Currently, we are observing between large time deltas between clinical processing of these patients and CDC's issuance of public warning.  It is our opinion that if A(H3N2)v suddenly displaces current seasonal A/H3N2 or gains significant prevalence, the first point of recognition may be an abruptly overwhelmed pediatric medical infrastructure versus dramatically time-delayed reporting from CDC. 

The observations of public health performance during the 2009 influenza pandemic begin to repeat themselves...

http://biosurveillance.typepad.com/biosurveillance/2011/12/more-evidence-of-human-human-transmission-of-swine-origin-triple-reassortant-influenza-ah3n2-virus-i.html

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