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Infectious Diseases Surveillance: Lessons Learned, Lessons to Learn .

PROF BECKIE NNENNA TAGBO (JP) MBBS, FCAI, FWACP (Paed), PhD, Vaccinology (Univ. Ghana & Cape Town), Advanced Vaccinology (Univ. Geneva), Epid Glob Health (Univ. Washington), Leadership & Mgt in Health (Univ. Washington), Glob Health Res (Univ. Washington)

✓ Director, Institute of Molecular Medicine and Infectious Diseases, College of Medicine, University of Nigeria.
✓ Professor of Paediatrics & Child Health, Department of Paediatrics, College of Medicine, University of Nigeria
✓ Chief Consultant Paediatrician, Department of Paediatrics/ Institute of Child Health, University of Nigeria teaching Hospital

• Chair of the WHO African Advisory Committee on Vaccine Safety (AACVS).
• Member, WHO (Global headquarters) Geneva, Global Advisory Committee on Vaccine Safety (GACVS) sub-committee on nOPV2 (novel oral polio vaccine type 2) Safety.
• Pioneered WHO AFRO / FED GOVT Rotavirus surveillance/ research for the first time in Nigeria in 2010 and thus headed the team that placed Nigeria on the World Health Organization Global map of rotavirus reporting countries of the world to WHO Global Headquarters at Geneva in 2010.
• Led the team that trained/established/mentored WHO AFRO Fed Govt/WHO AFRO rotavirus surveillance/research sites at UNTH Enugu(2010), UITH Ilorin(2013), ATBUTH Bauchi, ABUTH Zaria(both in Sept 2017).
• She has been involved in other new vaccines surveillance activities and has generated tremendous molecular/epidemiological data that has informed policy actions nationally and internationally.
• Site Coordinator for WHO AFRO intussusception and Paediatric Bacterial meningitis Sentinel Surveillance in Nigeria
• Principal investigator for several studies in infectious diseases
• Member, African Centre for Disease Control (CDC) Expert Committee for the development of the Pan-African Antimicrobial Standard Treatment Guidelines for Common Infections and Syndromes in Paediatric Patients.
• Fellow & Life member, West African College of Physicians (FWACP), in the Faculty of Paediatrics.
• Head, Paediatric Association of Nigeria Advisory Committee on Immunization from 2010 - 2022
• Member of many National working groups
• Member; National Ministerial Blueprint Committee on Routine Immunization.(As Immunization Field Expert)
• Member of 5 Working Groups of the GAIA/Brighton Collaboration
• Has vast experience in surveillance, research, policy meetings/consultation/special assignments, public health, vaccine clinical trial, immunization programme implementation /immunization training Consultant/Field Expert, advocacy, advisory committees,
• She is the Chief Editor of the 16-author Paediatric textbook titled “A Quick Glance at Paediatrics”
• Published many papers in both local and international high impact factor medical journals
• Journal Peer Reviewer for many journals
• Editorial Board Member for many journals

Awards
•Physician of the Year Award 2022 (Public sector)

Infectious Diseases Surveillance: Lessons Learned, Lessons to Learn .

PROF BECKIE NNENNA TAGBO (JP) MBBS, FCAI, FWACP (Paed), PhD, Vaccinology (Univ. Ghana & Cape Town), Advanced Vaccinology (Univ. Geneva), Epid Glob Health (Univ. Washington), Leadership & Mgt in Health (Univ. Washington), Glob Health Res (Univ. Washington)

✓ Director, Institute of Molecular Medicine and Infectious Diseases, College of Medicine, University of Nigeria.
✓ Professor of Paediatrics & Child Health, Department of Paediatrics, College of Medicine, University of Nigeria
✓ Chief Consultant Paediatrician, Department of Paediatrics/ Institute of Child Health, University of Nigeria teaching Hospital

• Chair of the WHO African Advisory Committee on Vaccine Safety (AACVS).
• Member, WHO (Global headquarters) Geneva, Global Advisory Committee on Vaccine Safety (GACVS) sub-committee on nOPV2 (novel oral polio vaccine type 2) Safety.
• Pioneered WHO AFRO / FED GOVT Rotavirus surveillance/ research for the first time in Nigeria in 2010 and thus headed the team that placed Nigeria on the World Health Organization Global map of rotavirus reporting countries of the world to WHO Global Headquarters at Geneva in 2010.
• Led the team that trained/established/mentored WHO AFRO Fed Govt/WHO AFRO rotavirus surveillance/research sites at UNTH Enugu(2010), UITH Ilorin(2013), ATBUTH Bauchi, ABUTH Zaria(both in Sept 2017).
• She has been involved in other new vaccines surveillance activities and has generated tremendous molecular/epidemiological data that has informed policy actions nationally and internationally.
• Site Coordinator for WHO AFRO intussusception and Paediatric Bacterial meningitis Sentinel Surveillance in Nigeria
• Principal investigator for several studies in infectious diseases
• Member, African Centre for Disease Control (CDC) Expert Committee for the development of the Pan-African Antimicrobial Standard Treatment Guidelines for Common Infections and Syndromes in Paediatric Patients.
• Fellow & Life member, West African College of Physicians (FWACP), in the Faculty of Paediatrics.
• Head, Paediatric Association of Nigeria Advisory Committee on Immunization from 2010 - 2022
• Member of many National working groups
• Member; National Ministerial Blueprint Committee on Routine Immunization.(As Immunization Field Expert)
• Member of 5 Working Groups of the GAIA/Brighton Collaboration
• Has vast experience in surveillance, research, policy meetings/consultation/special assignments, public health, vaccine clinical trial, immunization programme implementation /immunization training Consultant/Field Expert, advocacy, advisory committees,
• She is the Chief Editor of the 16-author Paediatric textbook titled “A Quick Glance at Paediatrics”
• Published many papers in both local and international high impact factor medical journals
• Journal Peer Reviewer for many journals
• Editorial Board Member for many journals

Awards
•Physician of the Year Award 2022 (Public sector)

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3.NISPID 2023 Pre-conference 2.pptx

  1. 1. NISPID 2023 Pre- conference Infectious Diseases Surveillance: Lessons Learned, Lessons to Learn 16-17 January 2023 Prof Beckie Tagbo • Director, Institute of Molecular Medicine and Infectious Diseases, College of Medicine, University of Nigeria & • Principal Investigator/ Site Coordinator, WHO/FGN New Vaccines (Disease( Surveillance
  2. 2. Why was it called 'surveillance'? • Close observation of exposed persons to identify onset of disease • Definition changed in the 1950s • What is the definition of public health surveillance? 2
  3. 3. Surveillance •Disease surveillance: The ongoing systematic collection and analysis of data and the provision of information which leads to action being taken to prevent and control a disease, usually one of an infectious nature. 3
  4. 4. What are the key elements of public health surveillance? • Ongoing • Systematic • Collection, analysis, interpretation, and dissemination • Data regarding a health-related event • For use in public health action to reduce morbidity and mortality and to improve health 4 http://www.cdc.gov/mmwr/preview/mmwrhtml/rr5013a1.htm You do not begin surveillance without the policy makers & implementers of response to outcomes
  5. 5. What types of surveillance strategies? •National and Sentinel (hospital- based) •Active and Passive •Indicator based and Event based Examples: •Polio •Measles •New vaccines 5
  6. 6. New Vaccines Surveillance: When and why? • Before vaccine introduction • Demonstrate disease burden • Justification to introduce vaccine • Establish system to measure vaccine impact • Identify circulating strains • After vaccine introduction • Monitor vaccination program impact • Monitor any change in circulating strains: needs strong laboratory support • Platform to evaluate safety 6 (i.e., surveillance for dxs targeted by new vaccines) E.g., Rotavirus & Paediatric Bacterial Meningitis surveillance
  7. 7. Sentinel vs. National Surveillance Sentinel: 1 Children's Hospital National: Every HCF, Every Case •Easier, cheaper •Likely good lab •Better quality data (active vs. passive) •Monitor trends over time •More severe cases, so not representative of all disease •More expensive, harder •Transport samples to lab •All disease in the country (mild, severe) •Monitor trends over time •Identify outbreaks, epidemics Spain Netherlands 7
  8. 8. NVS in Nigeria
  9. 9. Rotavirus Surveillance Countries Participatingin the WHO Network and Reporting Data for 2009 45 Data collected from WHO Regions and partners. Slide date: 22 June 2010 The boundaries and names shown and the designations used on this map do not imply the expression of any opinion whatsoever on the part of the World Health Organization concerning the legal status of any country, territory, city or area or of its authorities, or concerning the delimitation of its frontiers or boundaries. Dotted lines on maps represent approximate border lines for which there may not yet be full agreement. ©WHO 2010. All rights reserved Yes (55 Member States or 28%) Nigeria not reporting any data on rotavirus to WHO Geneva indicated by plain colour on the map
  10. 10. Rotavirus Surveillance Countries Participating in the WHO Network and Reporting Data for 2010 Data collected from WHO Regions. Slide date: 2 August 2010 Yes (55 Member States or 28% of Member States) 46 Nigeria, represented by ICH UNTH Enugu Site, now reporting data on rotavirus surveillance to WHO Geneva; indicated by blue colour on the map
  11. 11. There were challenges • We took a big chance, but God gave us favour • Govt & WHO came and saw our commitment and readiness • We were adopted • We trained/ established UITH, then Zaria & Bauchi >>> one big family • We did not just do data,… • Consistently committed to strong evidence-based advocacy/ sensitization/ awareness towards vaccine introduction • Vaccine should have been introduced much earlier…
  12. 12. There were challenges • Government had her own challenges too • Competing diseases and other aspects of health • Apart from bureaucratic bottlenecks… • Gavi application process… almost through… • Vaccine brand had supply capacity issues – birth cohort - 7m • Started Gavi process almost all over again • Then COVID-19 struck • Finally got Gavi approval and in Aug 2022, RV was launched (Northern states), & Dec 2022 for Southern states • Great story of eventual success • RV in private market costs about N5,000-N30,000 per dose! 12
  13. 13. Some WHO Prequalified Rotavirus Vaccines 13 NPHCDA Training Manual 2022
  14. 14. ROTAVAC 14 NPHCDA Training Manual 2022
  15. 15. Characteristics of Rotavac 15 NPHCDA Training Manual 2022
  16. 16. Characteristics of Rotavac 16 NPHCDA Training Manual 2022
  17. 17. Characteristics of Rotavac 17
  18. 18. Rotavirus vaccine launch!
  19. 19. Rotavirus vaccine launch! 19
  20. 20. Rotavirus vaccine launch 20
  21. 21. Current Rotavirus Vaccine Introduction Status 21 As of January 2022, 114 countries have introduced rotavirus vaccines
  22. 22. 22 Previous Rotavirus Vaccine Introduction Status
  23. 23. 23 Always ask to see the immunization card during clerking & indicate in your hx if card was sighted. Tell mother to ALWAYS bring it whenever bringing child to hospital for any ill-health. Nigerian national routine immunization schedule (by age) Revised Routine Immunization Schedule
  24. 24. Current Rotavirus Vaccine Introduction Status • More than 70% of countries in sub-Saharan Africa have introduced rotavirus vaccines. • But because rotavirus disease burden is so high in this region—more than half of all rotavirus deaths occur in African countries—it is critical that the remaining countries introduce vaccines to protect their children from rotavirus. 24
  25. 25. 25 Remember that vaccination is to be done in addition to all other existing measures
  26. 26. Nigeria Sentinel site surveillance for Rotavirus •Enugu (UNTH) - 2010 •Ilorin (UITH) - 2012 •Zaria (ABUTH) - 2017 •Bauchi (ATBUTH) – 2017 •Ilorin, Zaria and Bauchi sites were established and mentored by Enugu site 26 Lagos (LUTH) was scheduled for training in Dec 2022, but could not hold due to logistics issues
  27. 27. Rotavirus surveillance shifts to vaccine impact monitor and safety surveillance • We have therefore, commenced impact studies and case- controlled series safety study of a projected sample size of 800 • Before vaccine introduction • Demonstrate disease burden • Justification to introduce vaccine • Establish system to measure vaccine impact • Identify circulating strains • After vaccine introduction (Rotavac) • Monitor vaccination program impact • Monitor any change in circulating strains: needs strong laboratory support • Platform to evaluate safety New Vaccines Surveillance: When and why?
  28. 28. OUR DATA (ENUGU) 28
  29. 29. Publications
  30. 30. Our Data from 2010 to 2022 • Total Number of cases enrolled from inception = 5148 • Number positive =2262 • Percentage positivity = 44% • Chronic cases =32 • Bloody Cases =64
  31. 31. Male, 2288 44.4% Female, 2838 55.6% # Enrolled based on gender 2010-OCT 2022 (n=5126) Male, 1342 59.6% Female, 917 40.6% RV Positivity based on gender 2010-OCT 2022 (n=5126)
  32. 32. 0.00 10.00 20.00 30.00 40.00 50.00 60.00 70.00 0 100 200 300 400 500 600 700 2010201120122013201420152016201720182019202020212022 % Positivity No of Cases Annual Positivity of Rotavirus 2010-Oct 2022 # Enrolled # Positive % Positivity
  33. 33. 0 50 100 150 200 250 300 2010_10 2011_02 2011_06 2011_10 2012_02 2012_06 2012_10 2013_02 2013_06 2013_10 2014_02 2014_06 2014_10 2015_02 2015_06 2015_10 2016_02 2016_06 2016_10 2017_02 2017_06 2017_10 2018_02 2018_06 2018_10 2019_02 2019_06 2019_10 2020_02 2020_06 2020_10 2021_02 2021_06 2021_10 2022_02 Total vs Positive # Enrolled # Positive
  34. 34. 86.00 88.00 90.00 92.00 94.00 96.00 98.00 100.00 0 100 200 300 400 500 600 700 2010 2011 2012 2013 2014 2015 2016 2017 2018 2019 2020 2021 2022 Percentage of samples collected witin 48 hours # of Cases Annual Distribution of samples collected within 48hours of presentaion (Target=90%) # Enrolled Collected within 48hrs % collected within 48hrs Target 90%
  35. 35. 1 2 3 5 7 7 7 9 5 8 10 1 3 0.00 0.50 1.00 1.50 2.00 2.50 3.00 3.50 0 2 4 6 8 10 12 2010 2011 2012 2013 2014 2015 2016 2017 2018 2019 2020 2021 2022 % Case Fatality # of Fatality Annual Case Fatality 2010-Oct 2022 (n=66, 1.3%) No of deaths Case Fatality
  36. 36. Chronic / Pesistent Diarrhoea = 35, 36% Bloody Diarrhoea =62 64% Proportion of Bloody and Chronic diarrhoea cases collected from 2017 to Oct 2022 TaqMan Array Cards are high-throughput, accurate, sensitive, and simple-to-use tools for quantitative analysis of mRNA or miRNA transcripts using a real-time PCR protocol. They utilize a microfluidic card with 384 reaction chambers and eight sample loading ports. Interesting findings and the industry is already working on candidate vaccines… In one study, we tested for 35 organisms at once: 15 bacteria, 17 viruses, 1 fungus and 2 protozoan
  37. 37. Nigeria Sentinel site surveillance for Paediatric Bacterial Meningitis (PBM) • Lagos (LUTH) • Enugu (UNTH) • Ilorin (UITH) • Benin (UBTH) • Bauchi (ATBUTH) • Ilorin, Zaria and Bauchi have been integrated into the Enhanced Meningitis Surveillance 37 • Before vaccine introduction • Demonstrate disease burden • Justification to introduce vaccine • Establish system to measure vaccine impact • Identify circulating strains • After vaccine introduction (Rotavac) • Monitor vaccination program impact • Monitor any change in circulating strains: needs strong laboratory support • Platform to evaluate safety New Vaccines Surveillance: When and why?
  38. 38. Paediatric bacterial meningitis surveillance in Nigeria, from 2010 to 2016 Tagbo BN, Bancroft R, Fajolu I, Abdulkadir MB, Bashir MF, Okunola P, Isiaka A, Namadi L, Edelu BO, Onyejiaka N, Ihuoma CJ, Ndu F, Ozumba UC, Udeinya F,Ogunsola F, Saka AO, Fadeyi A , Aderibigbe SA, Abdulraheem J, Yusuf AG, Ogbogu P, Kanu C, Emina V, Makinwa J, Gehre F, Yusuf K, Braka F, Mwenda JM, Ticha JM, Nwodo D, Biey JN, Kwambana-Adams BA, Antonio M, for the African Paediatric Bacterial Meningitis Surveillance Network
  39. 39. Background •Historically, Nigeria has experienced large bacterial meningitis outbreaks causing high morbidity and mortality in children <5 years old. •Streptococcus pneumoniae, Neisseria meningitidis, and Haemophilus influenzae are the predominant causes of this invasive disease (using meningitis as proxy) which are preventable by immunization. •(Men:Pneumo >> 1:>9)
  40. 40. Background • In collaboration with the World Health Organisation, we conducted a longitudinal surveillance study across five sentinel hospitals within Nigeria to establish the burden of bacterial meningitis, • Aimed at providing data that supported the decision to introduce the Pneumococcal Conjugate Vaccine (PCV) to Nigeria’s immunization program and monitor impact
  41. 41. Figure 1: A map of the 36 states within Nigeria, highlighting the 5 states in which the 5 sentinel hospitals are situated
  42. 42. Methods •From 2010 to 2016, Cerebrospinal Fluid (CSF) was collected from children <5 years, admitted to five sentinel Hospitals across Nigeria. •Microbiological and latex agglutination techniques were performed on samples to detect the presence of S.pneumoniae, N.meningitidis and H.influenzae. •Species-specific polymerase chain reaction (PCR), and serotyping/serogrouping, was conducted to determine specific causative agents.
  43. 43. Results •In total, 5134 children with suspected meningitis were enrolled at the five hospitals. •A higher percentage of IBD was observed in children with turbid CSF samples (10.5%) compared to those with clear CSF (2.2%). •The dominant pathogen was pneumococcus (46.4%), followed by meningococcus (34.6%) and H. influenzae (18.9%). •The case fatality rate for confirmed bacterial meningitis was 15%.
  44. 44. Results •Overall, 53.6% of the pneumococcal meningitis cases were caused by serotypes covered by the PCV vaccines. •The most prevalent meningococcal and H. influenzae strains were serogroup W and Hib respectively
  45. 45. Total Suspected Cases 5134 Culture Negative 4664 Culture Positive 53 Culture Not Done 126 Shipment to MRC Culture Positive 23 Received and PCR at MRC 1318 LUTH NM =15 SP = 16 HI = 7 ATBUTH NM =9 SP = 14 HI = 8 UITH NM =0 SP = 1 HI = 2 UNTH NM =1 SP = 4 HI = 0 UBTH NM =3 SP = 2 HI = 0 LUTH NM =0 SP = 4 HI = 2 ATBUTH NM =10 SP = 12 HI = 7 UITH NM =1 SP = 7 HI = 2 UNTH NM =2 SP = 6 HI = 0 UBTH NM =0 SP = 0 HI = 0 Culture Negative 1179 Culture Not Done 16 Culture at Sentinel site Others 291 Others 100 Many PCR positive cases were culture negative
  46. 46. BINAX Pastorex Culture PCR BINAX Pastorex Culture PCR Pastorex Culture PCR Pastorex Culture PCR 0 25 50 75 100 Distribution (%) Detected Not Detected All Pathogens S.pneumoniae N.meningitidis H.influenzae 3 15 110 580 4825 1322 580 4825 110 1322 580 4825 1322 580 4825 1322 29 37 13 28 13 5 11 17 3 33 53 82 Sensitivity of Diagnostic Tests Used Most organisms were identified by Pastorex & PCR
  47. 47. Distribution of Bacterial Meningitis per month January February M arch April M ay June July August Septem ber October Novem ber Decem ber 0 5 10 15 20 25 Number of Meningitis Cases per Month (n) S.pneumonaie N.meningitidis H.influenzae N. meningitidi s was more in the first half of the year
  48. 48. 2 0 1 0 2 0 1 1 2 0 1 2 2 0 1 3 2 0 1 4 2 0 1 5 2 0 1 6 0 2 4 6 8 10 0 2 4 6 8 10 Number of Meningitis Cases 1 4 5 6A/6B/6C/6D 14 18A/18B/18C/18F 19A 19F 23A 23F Non-Typeable PCV10 PCV13 7a. 2 0 1 3 2 0 1 4 2 0 1 5 2 0 1 6 0 2 4 6 8 10 Number of Meningitis Cases B C W Non-Groupable 7b. 2 0 1 2 2 0 1 3 2 0 1 4 2 0 1 5 2 0 1 6 0 2 4 6 8 10 Number of H.influenzae Cases Hia Hib Hic 7c. Prevalence of each Bacterium and their Serotypes/Serogroups Spn Nm Hi Spn: Apart from the Non-typable strains, majority were vaccine strains Nm: Serogroups vary by year
  49. 49. Recommendation •Due to Nigeria’s large population vaccine programs for preventing meningitis were introduced in phases. •Continued surveillance is required to estimate vaccine impact as coverage improves and to determine the distribution of serotypes/serogroups of the predominant meningitis-causing pathogens across Nigeria in the post-vaccine era.
  50. 50. Lessons learned
  51. 51. My description of disease surveillance •Disease Surveillance is simply: •How do I pick up disease occurrence/ outbreaks earliest? •How do I report / document earliest? •How do I make meaning out of the data? •How do I respond earliest? •How do I monitor to see it has been adequately addressed? •How do I maintain vigilance thereafter to pick subsequent occurrences/ outbreaks or even new diseases? •How do I carry out all these in a coordinated manner on a large scale/ country wide / region wide scale? How do I ensure that I continue to improve and adapt the entire system/process to emerging trends?
  52. 52. Arriving disease will not pre- announce itself! So, the way to pick it up is to put in place continuous, consistent, sensitive and untiring mechanisms and strategies Disease will not announce, “I am coming, station yourselves to pick me”
  53. 53. Keywords – Sensitive and Responsive Surveillance System (Quality) The 2 keywords are sensitivity and responsiveness on a background of inclusiveness or comprehensiveness Questions? How do we make surveillance more sensitive? How do we make it more responsive? How do we build capacity? Entire System • Processes • Human resources • Material resources/ infrastructure • Governance
  54. 54. DS system in Africa is relatively young Dx surveillance system in Africa is Relatively Young Still developing Has sub-optimal coverage >>> True disease burdens unknown?
  55. 55. Disease Surveillance system in Africa is young Outbreaks missed or detected late Responses not prompt / not properly coordinated Resource allocation low >> Political / public perception of need low?
  56. 56. A key lesson We can make it happen
  57. 57. The Nigerian partnership model NCDC Ebola response - received international commendation Improved upon for Covid19 response in Nigeria Risk perception is key Partnership with private sector was good But only a small percentage who met certain requirements (orientation, std of care, resources and FG support/ collaboration) which should be upscaled (no of private facilities involved) and expanded (diseases covered) Spoke and wheel
  58. 58. Other lessons • Local data is very important and better than extrapolation or assumptions • Local strains are also important and could differ significantly from globally common strains • Policy making should not only be evidence based but include local evidence • Helps monitor progress – burden, impact of control measures, strain replacement, dx agent replacement, platform for vaccine safety surveillance
  59. 59. How do you set up a public health surveillance system? Steps in planning a surveillance system 1.Establish surveillance objectives 2.Develop case definitions for target diseases 3.Determine data sources data-collection mechanism (type of system) 4.Determine data-collection instruments / tools 5.Field-test methods 6.Develop and test analytic approach 7.Develop dissemination mechanism 8.Assure use of analysis and interpretation
  60. 60. Lessons to learn Private sector is largely untapped in DS • Constitutes 33-60% of health facilities, >70% iof healthcare spending in Nigeria and cannot be ignored (60% of the population in Anambra) • How to fully integrate the private sector in DS Quality & Relevance • How to make surveillance more sensitive, responsive, comprehensive (every case), inclusive (no of disease covered) • More focus on disease elimination New / Emerging diseases • Heighten index of suspicion for outbreak of new diseases • Event surveillance, • One-health principle / orientation
  61. 61. Case studies-1 Background Population > 5million >60% of health services are provided by private health facilities weak collaboration between the private and public health sector The engagement of private sector health practitioners significantly improved Integrated Disease Surveillance and Response (IDSR). Methods To achieve this, a multipronged approach was used, including: Involvement of the private health sector groups in key sector stakeholder’s meetings, capacity building events and provision of working tools State training of 862 health care workers on IDSR with 30% from private sector Engagement of private sector stakeholders in strengthening disease surveillance and response yields results (Anambra state Southeast Nigeria
  62. 62. Case studies-1 Inclusion of private sector in grassroot Integrated Data validation meetings across the 21 LGAs/Districts Procurement / distribution of documentation tools to all functional health facilities including the privately owned ones Orientation of the Association of General and Private Medical Practitioners of Nigeria (AGPMPN) among others Done with funding support from the EU to WHO for implementing the project: “Strengthening the Nigerian Health System towards Achieving Universal Health Coverage” Results Since the beginning of the EU funded health systems strengthening intervention in the State, the capacity for disease detection, diagnosis, case management, stock management and documentation have improved Engagement of private sector stakeholders in strengthening disease surveillance and response yields results (Anambra state Southeast Nigeria July 2019
  63. 63. Case studies-1 Response rate in implementation of policies & standards increased. Knowledge on disease notification and response as well as data management capacity equally improved Number of private health facilities generating and reporting IDSR data moved from 48 in May 2018 to 165 in December 2018 Significant increase in the coverage of TB services from 180 facilities in 2017 to 323 by 2018 ending, representing a 45% increase compared to previous year Overall, 23% increase in TB cases detection by December 2018 (2,300) compared to 1,800 detected in the previous year  This achievement is an all-time high for Anambra and occurred within a few weeks of the IDSR capacity scale up and orientation of the AGPMPN Engagement of private sector stakeholders in strengthening disease surveillance and response yields results (Anambra state Southeast Nigeria July 2019
  64. 64. Case studies-2 Background To explore evidence regarding the involvement of private practitioners in routine disease notification Method Systematic review, Search of databases, 40 papers reviewed Results Low private sector participation Main barriers - inadequate knowledge, unsatisfactory attitudes and misperceptions that influence practices Complex reporting system with unclear guidelines Unsatisfactory attitudes of public sector program staff Infrastructural barriers e.g., unavailability of computers Inadequate skilled human resources Conclusion Periodic training, supportive supervision and regular feedback to both public and private sectors in order to improve case notification. Governments – provide leadership, foster public-private collaborative partnerships, regulatory role From habits of attrition to modes of inclusion: enhancing the role of private practitioners in routine disease surveillance. Phalkey RK et al
  65. 65. Case studies-3 Background Assessed knowledge and practice of the private health-care facilities in DSN and explored models for private sector engagement in DSN in Southwestern Nigeria Methods Descriptive cross-sectional, using a semi-structured self-administered questionnaire Medical directors of 60 private health-care facilities in Osun State Results 53.3% ever notified LGA authorities 38.3% of facilities notified in the last 3 months 90.0% were willing to participate with Govt 15.0% regularly shared data with government monthly Predictors of good notification practice include: Having good knowledge of DSN Having received feedback from government or notified centers Having a designated DSN officer Conclusions High awareness and knowledge but poor practices of DSN were recorded Knowledge and practice of disease notification among private medical practitioners in Osun State, Southwestern Nigeria . Adebimpe W & Oluremi A
  66. 66. Case studies-4 Background: In Nigeria, private health facilities make up 33% of health facilities, >70% of healthcare spending, and >60% of healthcare contacts However, level of participation in DS system has been questioned Methods: Cross-sectional survey 507 private health facilities in South-West Nigeria (6 states) Investigate the level of compliance with disease surveillance reporting Factors that affect their participation Results: 40% of the private health facilities complied with routine DS reporting (17% to 60% across the 6 states in the zone) 34% had data collection tools, Compliance with disease surveillance and notification by private health providers in South-West Nigeria Makinde et al.
  67. 67. Case studies-4 49% had designated professionals assigned to health records management Only 7% of the clinicians could properly identify the data tools Predictive factors to compliance with disease surveillance participation included: Awareness of a law on disease surveillance (OR=1.55 95% CI=1.08-2.24), Availability of reporting tools (OR=13.69, 95% CI=8.85-21.62), Availability of a designated health records officer (OR=3.9, 95% CI=2.68-5.73), Health records officers (OR=10.51, 95%CI=2.86-67.70) and clinicians (OR=2.49, 95% CI=1.22-5.25) with knowledge of DS Conclusion Private health facilities were poorly compliant with disease surveillance resulting in missed opportunities for prompt identification and response to threats of disease outbreaks Makinde et al. Compliance with disease surveillance and notification by private health providers in South- West Nigeria. Pan African Medical Journal. 2020;35:114. [doi: 10.11604/pamj.2020.35.114.21188]
  68. 68. Starting steps… Develop a roadmap with incremental targets of private sector coverage/ disease coverage Private sector involvement must be wholesome starting from planning stages…case definitions, etc. Sustainable funding strategis too!
  69. 69. DS & R is developing in Africa Gross under-reporting especially from private sector Government stewardship / leadership is key Sensitive & responsive, quality inclusive/comprehensive DS Generate and apply evidence based boosting strategies Sustainable funding strategies Develop a comprehensive roadmap / framework Summary / Way forward
  70. 70. References NCDC. Strategies to improve surveillance for COVID-19, guidance for states NCDC. Integration of private sector laboratories in national COVID-19 response Ahmadi et al. Disease Surveillance and Private Sector in the Metropolitans: A Troublesome Collaboration. Int J Prev Med 2013;4:1036-44. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3793485/pdf/IJPVM-4-1036.pdf Kumar A, Furtado KM. Disease Surveillance: Engaging the Private Sector - The National Institution for Transforming India (NITI Aayog) https://www.niti.gov.in/sites/default/files/2019-01/Disease_surveillance_pvtsector.pdf Engagement of private sector stakeholders in strengthening disease surveillance and response yields results (Anambra state South East Nigeria July 2019 https://www.niti.gov.in/sites/default/files/2019-01/Disease_surveillance_pvtsector.pdf Anambra State Strategic Health Development Plan II, 2018 – 2022 From habits of attrition to modes of inclusion: enhancing the role of private practitioners in routine disease surveillance Revati K. Phalkey et al Adebimpe W & Oluremi A. Knowledge and practice of disease notification among private medical practitioners in Osun State, Southwestern Nigeria Nig J Clin Pract. 2019;17 Makinde et al. Compliance with disease surveillance and notification by private health providers in South-West Nigeria. Pan African Medical Journal. 2020;35:114. [doi: 10.11604/pamj.2020.35.114.21188] Available online at: https://www.panafrican- med-journal.com/content/article/35/114/full
  71. 71. Thank you and God bless Jesus saves WHO New Vaccines (Disease) Surveillance Team

Hinweis der Redaktion

  • 30 January 2023
  • Inclusive – as many diseases as possible
    Comprehensive – coverage, all cases including private sector and rural communities

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