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 Testing newborns for a handful of specific childhood conditions is
already commonplace in the U.S. "Newborn screening is often done
without parental permission and has been justified on the grounds
that the direct benefits to the child greatly outweigh the harms,"
said Dr. Lainie Friedman Ross of the MacLean Center for Clinical
Medical Ethics at the University of Chicago in Illinois, who
co-authored the case study in Pediatrics, November 12.
However, these tests are done to identify conditions that can be
diagnosed and treated early.
Sequencing all or large parts of a baby's genome at birth could
reveal genetic variations that increase risk for conditions that
occur in childhood or not until adulthood. The conditions could be
benign or ultimately be untreatable later, Ross said.
"To justify screening all infants in mandatory programs, we need to
ensure that the benefits greatly outweigh the harms, and we cannot
say this is the case for many of the variants we will identify by
sequencing," she told Reuters Health by email.
In 2014, the National Institutes of Health funded four projects to
study the benefits and risks of genomic sequencing for newborns. One
of them, the BabySeq Project, explored the medical, behavioral and
economic impacts of sequencing. As part of that clinical trial, half
of the babies were randomly assigned to receive sequencing along
with usual care. And parental consent included an agreement to
receive any results related to childhood-onset conditions.
During the study, however, a sequencing report showed that one baby
carried a BRCA2 mutation, which can be associated with an increased
risk of breast cancer. Although the family didn't have a history of
breast cancer, the research team felt moral distress about not being
able to disclose the information because it wasn't related to a
childhood disease.
The BabySeq researchers approached their institutional review board
and asked for permission to disclose it and then told the baby's
parents. Ultimately, the study protocol was modified to require all
participating families to agree to receive information about
adult-onset conditions, too.
When Ross and co-author Dr. Ellen Wright Clayton of the Vanderbilt
University Medical Center in Nashville, Tennessee, read about the
dilemma and the protocol change, they thought the decisions were
morally problematic.
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"If we do research on our children, we need to consider what rights
they have to privacy (particularly about information that will not
be relevant until they are adults) and what harms as well as what
benefits may accrue from seeking out this information years or
decades before it is necessary," Ross said.
Generally, professionals in the pediatric, genetics and ethics
communities agree that children shouldn't be tested for
adult-onset-only conditions, Ross and Clayton write. One argument
against testing for adult risk emphasizes the child's right to an
"open future" and to make the choice as an adult about what they
want to know.
The BabySeq researchers asserted that if the mother's life might be
saved by learning she is at increased risk for cancer, then the
whole family, including the infant, benefits from having her alive,
and that may outweigh other harms. But Ross and Clayton reject the
argument for a "family benefit."
"Until sequencing is ready for prime-time, the focus of pediatric
sequencing should be exclusively on identifying diseases or
conditions that can impact their present-day medical care," Ross
said.
In addition, questions about equity, access and affordability for
future treatments or preventive measures arise, bioethicist Aaron
Goldenberg of Case Western Reserve University in Cleveland, Ohio,
writes in an accompanying editorial.
Medical professionals should avoid making assumptions about how
patients from underserved communities may view these results, he
writes, especially if the results could be used in discriminatory
ways by future employers or insurance companies.
"It is crucial that this research include the potentially unique
concerns and considerations within underserved or underrepresented
communities," he told Reuters Health in an email. "We may be
reinforcing a system . . . (that) could ultimately exacerbate the
very health disparities we hope genomic medicine can help address."
SOURCE: https://bit.ly/2CGnXGA and https://bit.ly/352VB59 Pediatrics
2019.
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