As envisioned by Michael Boeckh, MD, PhD, head of Fred Hutch’s Infectious Disease Sciences Program, the two-day symposium was both a scientific conference and an opportunity “to train the next generation of leaders, researchers and clinicians” in this specialized field.
Seventy-one promising, early career doctors and scientists attended with full travel grants. Senior researchers and physicians who spoke at the gathering served as mentors to the trainees throughout the event.
“We invited both leaders in the field, but also the rising stars to hear about their research and their interpretation of the science,” Boeckh said as he opened the Seattle event on May 1.
Although the catastrophe of COVID-19 was seldom out of mind, speakers noted that the field was once again turning to what passed for normal before the pandemic: acute concern about the panoply of other microbial threats to patients.
For cancer patients, and for those recovering from either bone marrow or solid organ transplantation, the list of potentially lethal microbes is a lengthy one, often including influenza and germs that pose little threat to people with healthy immune systems: cytomegalovirus, parainfluenza, human herpesvirus-6 (it causes roseola in infants), and rhinoviruses, which cause the common cold.
The broad sweep of the symposium included talks on fungal infections and the dearth of good drugs to treat them; a discussion about modifying communities of gut bacteria — the microbiome — to combat multidrug resistant organisms; the use of laboratory-grown (monoclonal) antibody drugs to protect patients recovering from transplant; and a report raising concerns that recipients of advanced CAR-T cell therapies to treat certain blood cancers may need extra protection from microbial infections.
Janet Englund, MD, director of pediatric transplant infectious diseases at Seattle Children’s Hospital, said one enduring lesson of the pandemic was that extra doses of vaccines seemed to increase protection for many members of this vulnerable population, without increased risks of side effects, according to recent studies.
“More doses are better,” she said. “This is really pretty simple: we want more doses. Two doses are not enough in our immunocompromised patients, three doses are not enough in our immunocompromised children for sure, and four doses are really quite good.”
Englund echoed the calls to include the immunocompromised population in clinical trials, citing 10 years of failed efforts to test better monoclonal antibodies against respiratory syncytial virus in children. Pediatric transplant surgeons would love to give such drugs to children as a precaution prior to their transplants.
“It’s only going to change by us investigators writing and clamoring and begging and being obnoxious to the pharmaceutical companies,” she said.
Englund recognized, however, that drugmakers are concerned that adding riskier patients to a trial can make winning Food and Drug Administration approval more difficult, should a participant die in a trial, and that regulators should understand this.
“Our government agencies don’t appreciate how much we need to do these trials,” Englund added.