Live, Genetically Attenuated, Cold-Chain-Free Cholera Vaccine-A Research and Development Journey: Light at the End of a Long Tunnel

Manickam Ravichandran; Hui Xian Tew; Guruswamy Prabhakaran; Subramani Parasuraman; Mohd Nor Norazmi

doi:10.21315/mjms2022.29.2.1

Live, Genetically Attenuated, Cold-Chain-Free Cholera Vaccine-A Research and Development Journey: Light at the End of a Long Tunnel

Malays J Med Sci. 2022 Apr;29(2):1-7. doi: 10.21315/mjms2022.29.2.1. Epub 2022 Apr 21.

Authors

Manickam Ravichandran¹, Hui Xian Tew², Guruswamy Prabhakaran¹, Subramani Parasuraman³, Mohd Nor Norazmi^{1

4}

Affiliations

¹ Centre of Excellence for Vaccine Development (CoEVD), Faculty of Applied Sciences, AIMST University, Kedah, Malaysia.
² Faculty of Applied Sciences, AIMST University, Kedah, Malaysia.
³ Centre of Excellence for Vaccine Development (CoEVD), Faculty of Pharmacy, AIMST University, Kedah, Malaysia.
⁴ School of Health Sciences, Universiti Sains Malaysia, Kelantan, Malaysia.

Abstract

Cholera, a diarrheal disease caused by Vibrio cholerae (V. cholerae) O139 and O1 strains, remains a public health problem. The existing World Health Organization (WHO)-licenced, killed, multiple-dose oral cholera vaccines demand 'cold-chain supply' at 2 °C-8 °C. Therefore, a live, single-dose, cold-chain-free vaccine would relieve significant bottlenecks and costs of cholera vaccination campaigns. Our cholera vaccine development journey started in 2000 at Universiti Sains Malaysia with isolation of the hemA gene from V. cholerae, followed by development of a gene mutant vaccine candidate VCUSM2 against V. cholerae O139 in 2006. In 2010, VCUSM2 reactogenicity was reduced by replacing its two wild-type ctxA gene copies with mutated ctxA to produce strain VCUSM14. Introducing the hemA gene into VCUSM14 created VCUSM14P, a strain with the 5-aminolaevulinic acid (ALA) prototrophic trait and excellent colonisation and immunological properties (100% protection to wild-type challenged rabbits). It was further refined in Asian Institute of Medicine, Science and Technology (AIMST University), with completion of single- and repeated-dose toxicity evaluations in 2019 in Sprague Dawley (SD) rats, followed by development of a novel cold-chain-free VCUSM14P formulation in 2020. VCUSM14P is unique for its intact cholera toxin B, a known mucosal adjuvant. The built-in adjuvant makes VCUSM14P an ideal vaccine delivery platform for emerging diseases (e.g. severe acute respiratory syndrome coronavirus 2 [SARS-CoV-2] and tuberculosis). Our vaccine formulation mimics natural infection, remains non-reactogenic and immunogenic in vivo, and protects against infection and disease. It will also cost less and be less cumbersome to distribute due to its stability at room temperature. These features could revolutionise the outreach of this and other vaccines to meet global immunisation programmes, particularly in low-resourced areas. The next stage of our journey will be meeting the requisite regulatory requirements to produce the vaccine for rollout to countries where it is most needed.

Keywords: 5-aminolaevulinic acid (ALA) auxotroph; cholera; cold-chain-free; hemA mutation; live attenuated; vaccine.

Publication types

Editorial