WHO Target Product Profile for Plague Vaccines (Draft)

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Transcription:

WHO Target Product Profile for Plague Vaccines (Draft) Karene Yeung Initiative for Vaccine Research Department of Immunization, Vaccines and Biologicals

Outline Background Purpose Target audience Development and consultative process Expertise of working group Draft of Target Product Profile 2

Background Bubonic and pneumonic plague Large plague reservoirs in African, Asian and South American continents Outbreaks Emergence of antibiotic-resistance strains WHO priorities for product development 3

Purpose Development of new-generation of plague vaccines o Recrudescence of plague outbreaks o Availability of new vaccine technologies o Biodefense concerns Set out preferred and minimal characteristics for the next-generation plague vaccines from a public health perspective 4

Target audience Vaccine scientists Product developers Manufacturers Funding agencies Policy makers 5

Development and consultative process Early Feb Mid Feb Development of 1 st draft of TPP internally Identification of working group (WG) members with a variety of expertise Collection of Declaration of Interests from WG Early Mar Mid Mar Late Mar Early Apr Mid Apr Review and feedbacks on 1 st draft of TPP by WG Discussion on 1 st draft of TPP and comments through a teleconference Development of 2 nd draft of TPP Review and feedbacks on 2 nd draft of TPP by WG Discussion on 2 nd draft of TPP and comments through a teleconference Development of 3 rd draft of TPP Public consultation on 3 rd draft of TPP through an online platform 6

Expertise of working group 1. Research and development expertise in bacteriology and immunology 2. Research and development expertise in assays and animal models 3. Vaccine efficacy and effectiveness 4. Epidemiology/ public health/ vaccine policy 5. Deployment expertise in relevant countries 6. Modelling expertise 7. High income country regulators 8. Outbreak response 9. Ethics 7

DRAFT TARGET PRODUCT PROFILE (TPP) FOR PLAGUE VACCINES 8

Strategies Reactive/ emergency use o To prevent plague in vaccinated individuals in the face of an outbreak o To interrupt chains of transmission to terminate outbreaks o Populations experiencing an outbreak o Populations at high risk for importation of plague cases from areas experiencing an outbreak Preventive/ prophylactic use o To protect populations living in areas where plague is endemic o Health care workers (HWCs) at particularly high risk of plague due to their profession 9

Vaccine characteristics 1. Indication for use 2. Target population 3. Safety/ reactogenicity 4. Measures of efficacy 5. Dose regimen 6. Durability of protection 7. Route of administration 8. Coverage 9. Product stability and storage 10. Co-administration with other vaccines 11. Presentation 12. Registration and Prequalification Reactive/ emergency use Preventive/ prophylactic use Preferred Critical/ Minimal Preferred Critical/ Minimal 10

Indication for use Preferred Critical or Minimal Preferred Critical or Minimal For active immunization of at-risk persons in the area of an on-going outbreak to protect against plague; to be used in conjunction with other control measures to curtail or end an outbreak. For active immunization of persons considered potentially at risk to protect against plague. Risk groups will include communities in endemic areas and certain HCWs 1. 1 HCWs at particularly high risk of plague due to their profession (e.g. HCWs in endemic areas, laboratory personnel, deployed international HCWs) 11

Target population Preferred Critical or Minimal Preferred Critical or Minimal All age groups 2,3,4 excluding infants. Suitable for administration to pregnant and lactating women and to immunodeficient persons. All age groups 2,3,4 potentially excluding infants, pregnant and lactating women, and immunodeficient persons at the time of initial authorization based on the safety profile of the vaccine in these special populations 5. All age groups 2,3,4. Suitable for administration to pregnant and lactating women and to immunodeficient persons. All age groups 2,3,4 excluding pregnant and lactating women and immunodeficient persons 6. 2 Plague has occurred in people of all ages (infants up to age 96) https://www.cdc.gov/plague/maps/index.html 3 Ju C, Liu Z, Zhang G et al. Epidemiological characteristics of human plague in different age groups in China from 1950-2012. Zhonghua Liu Xing Bing Xue Za Zhi 2014;35:101-103. 4 Migliani R, Chanteau S, Rahalison L et al. Epidemiological trends for human plague in Madagascar during the second half of the 20th century: a survey of 20900 notified cases. Tropical Medicine & International Health 2006;11:1228-1237. 5 This determination would rely on whether the vaccine benefit outweighs safety risks - similar to the minimal characteristics for other populations. As vaccine products are used in these populations and more data is generated on the safety profile for use in infants, pregnant and lactating women, and immunodeficient persons, the label should be updated accordingly. 12 6 Post-licensure studies including the assessment of immunogenicity in pregnant and lactating women and immunocompromised individuals are expected.

Safety/ reactogenicity Preferred Critical or Minimal Preferred Critical or Minimal Safety and reactogenicity sufficient to provide a highly favorable risk-benefit profile, ideally with only mild and transient adverse events related to vaccination and no serious adverse events related to vaccination with the vaccine or vaccine-platform, including in individuals with compromised immune function or when administered in pregnancy. Safety and reactogenicity whereby vaccine benefit clearly outweighs safety risks. Safety and reactogenicity at least comparable to WHOrecommended routine vaccines, ideally with only mild and transient adverse events related to vaccination and no serious adverse events related to vaccination with the vaccine or vaccine platform, including in individuals with compromised immune function or when administered in pregnancy. Safety and reactogenicity whereby vaccine benefit clearly outweighs safety risks. 13

Measures of efficacy Preferred Critical or Minimal Preferred Critical or Minimal At least 80% efficacy 7 in preventing bubonic and pneumonic forms of plague in the target population. Rapid onset of protective immunity (less than one week). At least 70% efficacy 7 in preventing bubonic and pneumonic form of plague predicted and stop transmission in the affected population. Rapid onset of protective immunity (less than 10 days). At least 80% efficacy 7 in preventing bubonic and pneumonic form of plague in the target population. At least 70% efficacy 7 in preventing bubonic and pneumonic form of plague in the target population. 7 Clinical investigation should include assessment of immunogenicity in pregnancy and among immunocompromised individuals to identify potentially clinically relevant differences. If demonstration of clinical efficacy is not feasible, immunogenicity and efficacy data generated in standardized and relevant animal models bridged with clinical immunogenicity may be considered. Passive therapy using human sera may also provide evidence of biological effect. If efficacy trials are not feasible, the predicted efficacy should be at the level specified for desired efficacy. 14

Dose regimen Preferred Critical or Minimal Preferred Critical or Minimal Single-dose regimen highly preferred. Primary series: no more than 2 doses, with preference for less than onemonth interval between doses and good protection after the first dose. Single-dose regimen highly preferred. Primary series: no more than 3 doses, and with preference for less than one-month interval between doses. 15

Durability of protection Preferred Critical or Minimal Preferred Critical or Minimal Confers protection of at least 2 years. Confers protection of at least one year. Confers long-lasting protection of 10 years or more following the primary series and can be maintained indefinitely by booster doses. Confers protection of at least 5 years after primary series and can be maintained indefinitely by booster doses. 16

Route of administration Preferred Critical or Minimal Preferred Critical or Minimal Oral or nonparenteral route. A route enabling rapid mass administration. A route enabling rapid mass administration. Where injection (IM or SC) is required, using standard volumes for injection as specified in programmatic suitability for prequalification. Oral or nonparenteral route. A route compatible with use in routine immunization programs. A route compatible with use in routine immunization programs. Where injection (IM, ID or SC) is required, using standard volumes for injection as specified in programmatic suitability for prequalification. IM=Intramuscular, ID=Intradermal; SC=Subcutaneous 17

Coverage Preferred Critical or Minimal Preferred Critical or Minimal Coverage against all plague strains. Coverage against the most common outbreak plague strains. Coverage against all plague strains. Coverage against plague strains circulating in the endemic areas. 18

Product stability and storage Preferred Shelf life of at least 5 years at 2-8 o C. Preferably thermostable at higher temperatures for several days. The need for a preservative is determined and any issues are addressed including absence of toxicity. Vaccine Vial Monitor (VVM): Proof of feasibility and intent to apply a VVM to the primary container. Vaccines that are not damaged by freezing temperatures (<0 o C) are preferred. Vaccines stable out of cold chain are preferred. If not, vaccines that can be delivered via the Controlled Temperature Chain are preferred 8. Critical or Minimal Shelf life of at least 12 months at -20 o C and one month at 2-8 o C. The need for a preservativ e is determined and any issues are addressed including absence of toxicity. Preferred Shelf life of at least 5 years at 2-8 o C. Preferably thermostable at higher temperatures for several days. The need for a preservative is determined and any issues are addressed including absence of toxicity. Vaccine Vial Monitor (VVM): Proof of feasibility and intent to apply a VVM to the primary container. Vaccines that are not damaged by freezing temperatures (<0 o C) are preferred. Vaccines stable out of cold chain are preferred. If not, vaccines that can be delivered via the Controlled Temperature Chain are preferred 8. 8 http://www.who.int/immunization/programmes_systems/supply_chain/resources/controlled-temperature-chain-faq.pdf Critical or Minimal Shelf life of at least 2 years at -20 o C and 6 months at 2-8 o C. The need for a preservative is determined and any issues are addressed including absence of toxicity. Vaccine Vial Monitor (VVM): Proof of feasibility and intent to apply a VVM to the primary distribution container. 19

Co-administration with other vaccines Preferred Critical or Minimal Preferred Critical or Minimal The vaccine will be given as a stand-alone product not co-administered with other vaccines. The vaccine can be co-administered with other vaccines. The vaccine will be given as a standalone product not co-administered with other vaccines. 20

Presentation Preferred Critical or Minimal Preferred Critical or Minimal If oral administration, mono-dose presentation in plastic tubes with a volume of 1-2 ml; or multi-dose (10-20) with a dropper presentation with a maximal dosage volume of 0.05 ml (1 drop) or 0.1 ml (2 drops); with favorable taste (e.g. sweet). If injectable administration, vaccine is provided as a liquid product in 10-dose presentation with a volume of 0.5 ml. Multi-dose presentations should be formulated, managed and discarded in compliance with WHO s multi-dose vial policy. If oral administration, monodose presentation in glass vial with a volume of 1-2 ml or multi-dose container with a dropper device with 10-20 doses. If injectable administration, vaccine is provided as a liquid or lyophilized product in mono-dose or multi-dose (10-20) presentations with a volume of 0.5 ml. Multi-dose presentations should be formulated, managed and discarded in compliance with WHO s multi-dose vial policy. If not supplied in a dualbarrel syringe, lyophilized vaccine will need to be accompanied by paired separate vials of the appropriate diluent. If oral administration, 2-5 doses with a volume of 1-2 ml in plastic tubes; with favorable taste (e.g. sweet). If injectable administration, vaccine is provided as a liquid product in mono-dose or multidose (2) presentations with a maximal dosage volume of 0.5 ml. Multi-dose presentations should be formulated, managed and discarded in compliance with WHO s multi-dose vial policy. If oral administration, 2-5 doses with a volume of 1-2 ml in plastic tubes. If injectable administration, vaccine is provided as a liquid or lyophilized product in mono-dose or multi-dose (5-10) presentations with a maximal dosage volume of 0.5 ml. Multi-dose presentations should be formulated, managed and discarded in compliance with WHO s multi-dose vial policy. If not supplied in a dualbarrel syringe, lyophilized vaccine will need to be accompanied by paired separate vials of the 21 appropriate diluent.

Registration and prequalification Preferred Critical or Minimal Preferred Critical or Minimal Should be WHO pre-qualified according to the process outlined in Procedures for assessing the acceptability, in principle, of vaccines for purchase by United Nations agencies. Should be WHO pre-qualified according to the process outlined in Procedures for assessing the acceptability, in principle, of vaccines for purchase by United Nations agencies. 22

THE END Thank you 23

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