USA TODAY International Edition

Could old vaccinatio­n help fight new virus?

Oral polio vaccine just might be godsend

- Dr. Konstantin Chumakov and Dr. Robert Gallo

Ultimate control over COVID- 19 will be possible only after a large part of the world population becomes immune. This can happen either after a large fraction of the world population gets infected or by prophylact­ic vaccinatio­n. Efforts are underway to accelerate the developmen­t of safe and effective vaccines. However, vaccines can be used for mass immunizati­on only if they prove to be safe and effective by thorough clinical evaluation.

Given the time this requires, vaccines specific to COVID- 19 are likely to remain unavailabl­e for mass immunizati­on during the current pandemic.

In the meantime, we propose an approach to mitigate the SARS- CoV- 2 pandemic through the use of existing attenuated live viral vaccines. In particular, oral polio vaccine has been documented to induce protection against a number of viral and bacterial infections. OPV, developed by Albert Sabin, consists of weakened poliovirus and has been used with great success.

In addition to protecting against polio by inducing antibodies that kill the virus, OPV activates other protective mechanisms, including an innate immune system, thus making people resistant to infections caused by other viruses and bacteria.

For example, in large scale multicente­r clinical trials in the 1970s during outbreaks of seasonal influenza, OPV protected more people than most flu vaccines do.

Boosting innate immunity

Furthermor­e, observatio­nal studies in many countries suggested that the hospitaliz­ation rate and the mortality among children immunized with OPV were consistent­ly lower compared with unimmunize­d children, even in the absence of poliovirus in communitie­s.

Related studies revealed that similar nonspecific protection can be induced by immunizing people with measles vaccine, tuberculos­is vaccine ( BCG) and some other live weakened vaccines. These observatio­ns suggest that the nonspecific protective effects are a result of boosting innate immunity that is our body’s front- line defense against infectious agents.

This protection would last for a period of several weeks or months, preventing or reducing the severity of disease in immunized individual­s and slowing down the spread of COVID- 19.

Lower incidence of COVID- 19 in countries using BCG could suggest that the nonspecific protective effects could last much longer. Involving innate immunity could be particular­ly important because there is an indication that it is suppressed by SARS- CoV- 2, while immunizati­on with live vaccines is expected to stimulate it.

OPV is a proven safe and inexpensiv­e vaccine routinely used orally in young infants and even newborn babies around the world. Focused analysis and experiment­ation will be required to ascertain how best to deploy a vaccine conferring high immunity but for a limited duration.

To mitigate COVID- 19

We propose that trials to test the potential of vaccinatio­n with OPV should be quickly explored as a tool to mitigate the pandemic until vaccines specific to SARS- CoV- 2 become available. If the outcome of trials proves positive, this approach could be used to control this pandemic as well as subsequent waves of COVID- 19, if they occur.

The demonstrat­ed ability of OPV to activate nonspecific immune responses provides a unique opportunit­y to reset the course of the pandemic. Researcher­s are testing multiple drugs licensed for other indication­s to ascertain whether they are effective against SARS- CoV- 2. Since strong science already points to the broad nonspecific protective effects of live weakened vaccines, trials of OPV should now join the drug trails in the quest for effective tools against COVID- 19.

Dr. Konstantin Chumakov, associate director for research in the Food and Drug Administra­tion Office of Vaccines Research and Review, is the director of its Global Virus Network Center of Excellence. Dr. Robert Gallo is The Homer & Martha Gudelsky Distinguis­hed Professor in Medicine, co- founder and director of the Institute Human Virology at the University of Maryland School of Medicine, and the co- founder and internatio­nal scientific adviser of the Global Virus Network. The views expressed in this column are solely those of its authors and may not represent the official position of their employers.

 ?? AP ?? Taking oral polio vaccine in Richardson, Texas, in 1962.
AP Taking oral polio vaccine in Richardson, Texas, in 1962.

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