Sisonke phase 3B open-label study: Lessons learnt for national and global vaccination scale-up during epidemics

A. E. Goga; L. G. Bekker; N. Garrett; S. Takuva; I. Sanne; J. Odhiambo; F. Mayat; L. Fairall; Z. Brey; L. Bamford; G. Tanna; G. Gray

doi:10.7196/SAMJ.2022.v112i2b.16098

Sisonke phase 3B open-label study: Lessons learnt for national and global vaccination scale-up during epidemics

A. E. Goga^*, L. G. Bekker, N. Garrett, S. Takuva, I. Sanne, J. Odhiambo, F. Mayat, L. Fairall, Z. Brey, L. Bamford, G. Tanna, G. Gray

^*Corresponding author for this work

Population Health Sciences

Research output: Contribution to journal › Article › peer-review

4 Citations (Scopus)

Abstract

Sisonke is a multicentre, open-label, single-arm phase 3B vaccine implementation study of healthcare workers (HCWs) in South Africa, with prospective surveillance for 2 years. The primary endpoint is the rate of severe COVID‑19, including hospitalisations and deaths. The Sisonke study enrolled and vaccinated participants nationally at potential vaccination roll-out sites between 17 February and 26 May 2021. After May 2021, additional HCWs were vaccinated as part of a sub-study at selected clinical research sites. We discuss 10 lessons learnt to strengthen national and global vaccination strategies:(i) consistently advocate for vaccination to reduce public hesitancy; (ii) an electronic vaccination data system (EVDS) is critical; (iii) facilitate access to a choice of vaccination sites, such as religious and community centres, schools, shopping malls and drive-through centres; (iv) let digitally literate people help elderly and marginalised people to register for vaccination; (v) develop clear 'how to' guides for vaccine storage, pharmacy staff and vaccinators; (vi) leverage instant messaging platforms, such as WhatsApp, for quick communication among staff at vaccination centres; (vii) safety is paramount - rapid health assessments are needed at vaccination centres to identify people at high risk of serious adverse events, including anaphylaxis or thrombosis with thrombocytopenia syndrome. Be transparent about adverse events and contextualise vaccination benefits, while acknowledging the small risks; (viii) provide real-time, responsive support to vaccinees post vaccination and implement an accessible national vaccine adverse events surveillance system; (ix) develop efficient systems to monitor and investigate COVID‑19 breakthrough infections; and (x) flexibility and teamwork are essential in vaccination centres across national, provincial and district levels and between public and private sectors.

Original language	English
Pages (from-to)	13486
Number of pages	1
Journal	South African Medical Journal
Volume	112
Issue number	2 b
DOIs	https://doi.org/10.7196/SAMJ.2022.v112i2b.16098
Publication status	Published - 24 Dec 2021

Keywords

COVID-19/prevention & control
COVID-19 Vaccines/administration & dosage
Health Personnel
Humans
Infectious Disease Transmission, Patient-to-Professional/prevention & control
Mass Vaccination
Prospective Studies
SARS-CoV-2
South Africa/epidemiology
Vaccination Hesitancy

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.7196/SAMJ.2022.v112i2b.16098

Cite this

@article{8e2ddd9cc18348ad874220802849085f,

title = "Sisonke phase 3B open-label study: Lessons learnt for national and global vaccination scale-up during epidemics",

abstract = "Sisonke is a multicentre, open-label, single-arm phase 3B vaccine implementation study of healthcare workers (HCWs) in South Africa, with prospective surveillance for 2 years. The primary endpoint is the rate of severe COVID‑19, including hospitalisations and deaths. The Sisonke study enrolled and vaccinated participants nationally at potential vaccination roll-out sites between 17 February and 26 May 2021. After May 2021, additional HCWs were vaccinated as part of a sub-study at selected clinical research sites. We discuss 10 lessons learnt to strengthen national and global vaccination strategies:(i) consistently advocate for vaccination to reduce public hesitancy; (ii) an electronic vaccination data system (EVDS) is critical; (iii) facilitate access to a choice of vaccination sites, such as religious and community centres, schools, shopping malls and drive-through centres; (iv) let digitally literate people help elderly and marginalised people to register for vaccination; (v) develop clear 'how to' guides for vaccine storage, pharmacy staff and vaccinators; (vi) leverage instant messaging platforms, such as WhatsApp, for quick communication among staff at vaccination centres; (vii) safety is paramount - rapid health assessments are needed at vaccination centres to identify people at high risk of serious adverse events, including anaphylaxis or thrombosis with thrombocytopenia syndrome. Be transparent about adverse events and contextualise vaccination benefits, while acknowledging the small risks; (viii) provide real-time, responsive support to vaccinees post vaccination and implement an accessible national vaccine adverse events surveillance system; (ix) develop efficient systems to monitor and investigate COVID‑19 breakthrough infections; and (x) flexibility and teamwork are essential in vaccination centres across national, provincial and district levels and between public and private sectors.",

keywords = "COVID-19/prevention & control, COVID-19 Vaccines/administration & dosage, Health Personnel, Humans, Infectious Disease Transmission, Patient-to-Professional/prevention & control, Mass Vaccination, Prospective Studies, SARS-CoV-2, South Africa/epidemiology, Vaccination Hesitancy",

author = "Goga, {A. E.} and Bekker, {L. G.} and N. Garrett and S. Takuva and I. Sanne and J. Odhiambo and F. Mayat and L. Fairall and Z. Brey and L. Bamford and G. Tanna and G. Gray",

note = "Funding Information: The Sisonke study team and collaborators made history by moving from the ENSEMBLE phase 3 trial results to the large‑scale phase 3B study in <2 months. The Sisonke study is an example of what is possible when political will, science, hard work, partnership and a strong desire to act come together to serve public health. Declaration. None. Acknowledgements. South African Medical Research Council (study sponsor and oversight), Janssen Vaccines and Prevention (supply and transport of the study product to South Africa), National Department of Health, overseeing ethics committees, South African Health Products Regulatory Authority, Biocair, vaccine centres (hospitals), clinical research site principal investigators and teams, including the following: S Badal‑ Faesen (Themba Lethu HIV Research Unit and Clinical HIV Research Unit (CHRU)), S Barnabas (FAM‑CRU), L G Bekker and S Mahoney (Desmond Tutu HIV Foundation‑Emavundleni Research Centre), L Burgess (TREAD Research), W Brumskine (Aurum Institute Rustenburg Clinical Research Centre), R Dawson (University of Cape Town Lung Institute), A Diacon (TASK Central), T Dubula (Nelson Mandela Academic Clinical Research Unit), J Engelbrecht (Dr J M Engelbrecht Clinical Trial Site), K Gill (Desmond Tutu Health Foundation (DTHF) Masiphumelele Clinic), C Grobbelaar (Aurum Institute Clinical Research Centre Pretoria), L Hellstrom (Be Part‑Yoluntu Centre), N Hussen (Worthwhile Clinical Trials), C Innes (Aurum Institute Klerksdorp Clinical Research Centre), N Joseph (Peermed CTC (Pty) Ltd T/A MERC), S Kassim (Desmond Tutu Health Foundation Clinical Trials Unit ), S Kotze (Synexus Stanza Research Centre), P Kotze (Qhakaza Mbokodo Research Clinic), E Lazarus (Perinatal HIV Research Unit), J Lombard (Josha Research), A Luabeya (South African Tuberculosis Vaccine Initiative (SATVI), Brewelskloof Hospital), D Makhaza (CAPRISA Vulindlela Clinic), R B Maboa (Ndlovu Research Centre), M Malahela (Setshaba Research Centre), D Malan (PHOENIX Pharma (Pty) Ltd), M Mamba (CRISMO Bertha Gxowa Research Centre), K Mngadi (Aurum Institute Tembisa Clinical Research Centre), L Naidoo (Chatsworth Clinical Research Site, SAMRC), N Naicker (CAPRISA eThekwini Clinic), V Naicker (Tongaat Clinical Research site, SAMRC), M Nchabaleng (Mecru Clinical Research Unit), T Nielsen (Aurum Institute), F Patel (Wits RHI‑ Shandukani Research), F Petrick (Mzansi Ethical Research Centre), E Spooner (Botha{\textquoteright}s Hill Clinical Research site, SAMRC), D Urbach (Synexus Helderberg Clinical Research Centre), E van Nieuwenhuizen (Synexus SA Watermeyer Clinical Research Centre ), A Ward (Ekhayavac TB Vaccine Trial Unit/Khayelitsha CRS (CIDRI UCT)). Author contributions. GG, L‑GB, AEG and NG conceptualised the Sisonke study. AEG wrote the first draft of the manuscript. All authors contributed to all sections of the article and reviewed the draft manuscript. Funding. The Sisonke study is funded by the South African Medical Research Council, with funds received from National Treasury through the South African National Department of Health and by the Solidarity Fund, the ELMA Vaccines and Immunisation Foundation, the Michael and Susan Dell Foundation and the Bill and Melinda Gates Foundation. Conflicts of interest. None. Publisher Copyright: {\textcopyright} 2022 South African Medical Association. All rights reserved.",

year = "2021",

month = dec,

day = "24",

doi = "10.7196/SAMJ.2022.v112i2b.16098",

language = "English",

volume = "112",

pages = "13486",

journal = "South African Medical Journal",

issn = "0256-9574",

publisher = "South African Medical Association",

number = "2 b",

}

TY - JOUR

T1 - Sisonke phase 3B open-label study

T2 - Lessons learnt for national and global vaccination scale-up during epidemics

AU - Goga, A. E.

AU - Bekker, L. G.

AU - Garrett, N.

AU - Takuva, S.

AU - Sanne, I.

AU - Odhiambo, J.

AU - Mayat, F.

AU - Fairall, L.

AU - Brey, Z.

AU - Bamford, L.

AU - Tanna, G.

AU - Gray, G.

N1 - Funding Information: The Sisonke study team and collaborators made history by moving from the ENSEMBLE phase 3 trial results to the large‑scale phase 3B study in <2 months. The Sisonke study is an example of what is possible when political will, science, hard work, partnership and a strong desire to act come together to serve public health. Declaration. None. Acknowledgements. South African Medical Research Council (study sponsor and oversight), Janssen Vaccines and Prevention (supply and transport of the study product to South Africa), National Department of Health, overseeing ethics committees, South African Health Products Regulatory Authority, Biocair, vaccine centres (hospitals), clinical research site principal investigators and teams, including the following: S Badal‑ Faesen (Themba Lethu HIV Research Unit and Clinical HIV Research Unit (CHRU)), S Barnabas (FAM‑CRU), L G Bekker and S Mahoney (Desmond Tutu HIV Foundation‑Emavundleni Research Centre), L Burgess (TREAD Research), W Brumskine (Aurum Institute Rustenburg Clinical Research Centre), R Dawson (University of Cape Town Lung Institute), A Diacon (TASK Central), T Dubula (Nelson Mandela Academic Clinical Research Unit), J Engelbrecht (Dr J M Engelbrecht Clinical Trial Site), K Gill (Desmond Tutu Health Foundation (DTHF) Masiphumelele Clinic), C Grobbelaar (Aurum Institute Clinical Research Centre Pretoria), L Hellstrom (Be Part‑Yoluntu Centre), N Hussen (Worthwhile Clinical Trials), C Innes (Aurum Institute Klerksdorp Clinical Research Centre), N Joseph (Peermed CTC (Pty) Ltd T/A MERC), S Kassim (Desmond Tutu Health Foundation Clinical Trials Unit ), S Kotze (Synexus Stanza Research Centre), P Kotze (Qhakaza Mbokodo Research Clinic), E Lazarus (Perinatal HIV Research Unit), J Lombard (Josha Research), A Luabeya (South African Tuberculosis Vaccine Initiative (SATVI), Brewelskloof Hospital), D Makhaza (CAPRISA Vulindlela Clinic), R B Maboa (Ndlovu Research Centre), M Malahela (Setshaba Research Centre), D Malan (PHOENIX Pharma (Pty) Ltd), M Mamba (CRISMO Bertha Gxowa Research Centre), K Mngadi (Aurum Institute Tembisa Clinical Research Centre), L Naidoo (Chatsworth Clinical Research Site, SAMRC), N Naicker (CAPRISA eThekwini Clinic), V Naicker (Tongaat Clinical Research site, SAMRC), M Nchabaleng (Mecru Clinical Research Unit), T Nielsen (Aurum Institute), F Patel (Wits RHI‑ Shandukani Research), F Petrick (Mzansi Ethical Research Centre), E Spooner (Botha’s Hill Clinical Research site, SAMRC), D Urbach (Synexus Helderberg Clinical Research Centre), E van Nieuwenhuizen (Synexus SA Watermeyer Clinical Research Centre ), A Ward (Ekhayavac TB Vaccine Trial Unit/Khayelitsha CRS (CIDRI UCT)). Author contributions. GG, L‑GB, AEG and NG conceptualised the Sisonke study. AEG wrote the first draft of the manuscript. All authors contributed to all sections of the article and reviewed the draft manuscript. Funding. The Sisonke study is funded by the South African Medical Research Council, with funds received from National Treasury through the South African National Department of Health and by the Solidarity Fund, the ELMA Vaccines and Immunisation Foundation, the Michael and Susan Dell Foundation and the Bill and Melinda Gates Foundation. Conflicts of interest. None. Publisher Copyright: © 2022 South African Medical Association. All rights reserved.

PY - 2021/12/24

Y1 - 2021/12/24

N2 - Sisonke is a multicentre, open-label, single-arm phase 3B vaccine implementation study of healthcare workers (HCWs) in South Africa, with prospective surveillance for 2 years. The primary endpoint is the rate of severe COVID‑19, including hospitalisations and deaths. The Sisonke study enrolled and vaccinated participants nationally at potential vaccination roll-out sites between 17 February and 26 May 2021. After May 2021, additional HCWs were vaccinated as part of a sub-study at selected clinical research sites. We discuss 10 lessons learnt to strengthen national and global vaccination strategies:(i) consistently advocate for vaccination to reduce public hesitancy; (ii) an electronic vaccination data system (EVDS) is critical; (iii) facilitate access to a choice of vaccination sites, such as religious and community centres, schools, shopping malls and drive-through centres; (iv) let digitally literate people help elderly and marginalised people to register for vaccination; (v) develop clear 'how to' guides for vaccine storage, pharmacy staff and vaccinators; (vi) leverage instant messaging platforms, such as WhatsApp, for quick communication among staff at vaccination centres; (vii) safety is paramount - rapid health assessments are needed at vaccination centres to identify people at high risk of serious adverse events, including anaphylaxis or thrombosis with thrombocytopenia syndrome. Be transparent about adverse events and contextualise vaccination benefits, while acknowledging the small risks; (viii) provide real-time, responsive support to vaccinees post vaccination and implement an accessible national vaccine adverse events surveillance system; (ix) develop efficient systems to monitor and investigate COVID‑19 breakthrough infections; and (x) flexibility and teamwork are essential in vaccination centres across national, provincial and district levels and between public and private sectors.

AB - Sisonke is a multicentre, open-label, single-arm phase 3B vaccine implementation study of healthcare workers (HCWs) in South Africa, with prospective surveillance for 2 years. The primary endpoint is the rate of severe COVID‑19, including hospitalisations and deaths. The Sisonke study enrolled and vaccinated participants nationally at potential vaccination roll-out sites between 17 February and 26 May 2021. After May 2021, additional HCWs were vaccinated as part of a sub-study at selected clinical research sites. We discuss 10 lessons learnt to strengthen national and global vaccination strategies:(i) consistently advocate for vaccination to reduce public hesitancy; (ii) an electronic vaccination data system (EVDS) is critical; (iii) facilitate access to a choice of vaccination sites, such as religious and community centres, schools, shopping malls and drive-through centres; (iv) let digitally literate people help elderly and marginalised people to register for vaccination; (v) develop clear 'how to' guides for vaccine storage, pharmacy staff and vaccinators; (vi) leverage instant messaging platforms, such as WhatsApp, for quick communication among staff at vaccination centres; (vii) safety is paramount - rapid health assessments are needed at vaccination centres to identify people at high risk of serious adverse events, including anaphylaxis or thrombosis with thrombocytopenia syndrome. Be transparent about adverse events and contextualise vaccination benefits, while acknowledging the small risks; (viii) provide real-time, responsive support to vaccinees post vaccination and implement an accessible national vaccine adverse events surveillance system; (ix) develop efficient systems to monitor and investigate COVID‑19 breakthrough infections; and (x) flexibility and teamwork are essential in vaccination centres across national, provincial and district levels and between public and private sectors.

KW - COVID-19/prevention & control

KW - COVID-19 Vaccines/administration & dosage

KW - Health Personnel

KW - Humans

KW - Infectious Disease Transmission, Patient-to-Professional/prevention & control

KW - Mass Vaccination

KW - Prospective Studies

KW - SARS-CoV-2

KW - South Africa/epidemiology

KW - Vaccination Hesitancy

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U2 - 10.7196/SAMJ.2022.v112i2b.16098

DO - 10.7196/SAMJ.2022.v112i2b.16098

M3 - Article

C2 - 35140006

AN - SCOPUS:85124625508

SN - 0256-9574

VL - 112

SP - 13486

JO - South African Medical Journal

JF - South African Medical Journal

IS - 2 b

ER -

Sisonke phase 3B open-label study: Lessons learnt for national and global vaccination scale-up during epidemics

Abstract

Keywords

UN SDGs

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