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The evolution of vaccine developments, from small pox to COVID-19
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The evolution of vaccine developments, from small pox to COVID-19
Thu, 2021-04-01 21:00 — mike krafthttps://www.nejm.org/doi/full/10.1056/NEJMp2034334
On the Shoulders of Giants — From Jenner’s Cowpox to mRNA Covid Vaccines
In September 2008, Katalin Karikó, Drew Weissman, and their colleagues at the University of Pennsylvania modified messenger RNA (mRNA) using nucleoside analogues. These modifications stabilized the molecule and eliminated its capacity for inducing innate immunity, thereby making mRNA a promising tool for both gene replacement and vaccination.1 In December 2020, on the basis of safety and efficacy data generated in two large, placebo-controlled studies, the Food and Drug Administration (FDA) issued emergency use authorizations for two mRNA vaccines for the prevention of Covid-19. Clearance of this hurdle by the first mRNA vaccines represents the most recent in a series of breakthroughs in the realm of viral vaccines, each building on the last and each with a compelling record of disease prevention.
The first major vaccine-related advance occurred in 1796, when Edward Jenner, a physician working in southern England, found that an animal virus (cowpox) could protect against disease caused by a human virus (smallpox).2 One hundred years would pass before viruses would be identified as causative agents of disease; nevertheless, the notion that infectious diseases could be prevented by vaccination was born. Jenner’s work ultimately led to the eradication of a disease that is estimated to have killed more than 300 million people in the 20th century. The strategy of using animal viruses to prevent human diseases continues today with a rotavirus vaccine that is derived in part from a bovine strain of the virus.
The second breakthrough occurred nearly a century after the first. In 1885, Louis Pasteur found that the spinal cords of rabbits that had been experimentally inoculated with rabies virus were no longer infectious after 15 days of desiccation.3 On July 6, 1885, Joseph Meister, a 9-year-old boy who had been attacked by a rabid dog 2 days earlier, visited Pasteur’s laboratory. Using a series of inoculations with suspensions of desiccated rabbit spinal cords, Pasteur saved Meister’s life. Rabies, a disease with a mortality of virtually 100%, was now preventable after exposure. Pasteur had opened the door for vaccines made with physically or chemically inactivated viruses. During the 20th century, notable successes that relied on the killed-virus strategy included an influenza vaccine developed by Thomas Francis in the early 1940s, a polio vaccine developed by Jonas Salk in the mid-1950s (Salk had trained in Francis’s laboratory at the University of Michigan), and a hepatitis A vaccine developed by Philip Provost and Maurice Hilleman in 1991.
The third major advance in vaccinology occurred in 1937, when Max Theiler attenuated yellow fever virus by means of serial passage in mouse and chicken embryos.4 By forcing the virus to grow in nonhuman cells, Theiler introduced a series of blind genetic alterations in the virus that rendered it less capable of causing disease but still capable of inducing protective immunity. For this work, Theiler was awarded the 1951 Nobel Prize in Physiology or Medicine. Derivatives of Theiler’s yellow fever vaccine are still used today. The latter half of the 20th century witnessed an explosion of live attenuated viral vaccines developed using his technique. In the early 1960s, Albert Sabin, who had trained in Theiler’s laboratory at the Rockefeller Foundation in New York City, made a polio vaccine by weakening polio viruses using serial passage in monkey kidney and testicular cells. Other live attenuated vaccines followed, including vaccines to prevent measles (1963), mumps (1967), rubella (1969), varicella (1995), and rotavirus (2008). ...
The fourth breakthrough occurred in 1980, when Stanford biochemists Richard Mulligan and Paul Berg published findings from their experiments that involved transfecting monkey kidney cells with an Escherichia coli gene and thereby causing mammalian cells to make a bacterial protein.5 Recombinant DNA technology was born. Made using yeast or baculovirus-expression systems, vaccines containing purified surface proteins from hepatitis B virus (1986), human papillomavirus (2006), and influenza virus (2013) have since become available.
Although there is still much work to be done to address vaccine hesitancy, build trust, and ensure equitable benefits from vaccination, the list of vaccine successes in the United States is long. After the introduction of Salk’s inactivated polio vaccine, for example, the incidence of polio dropped from 29,000 cases in 1955 to fewer than 900 in 1962. With the introduction of Sabin’s live attenuated vaccine in the early 1960s, polio was eliminated from the United States. Since its licensure in 2006, the bovine–human reassortant rotavirus vaccine has virtually eliminated rotavirus, preventing up to 75,000 hospitalizations and 60 deaths per year. During the 2019–2020 influenza season, the influenza vaccine prevented an estimated 7.52 million infections, 3.69 million medical visits, 105,000 hospitalizations, and 6300 deaths in the United States.
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