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Transcript 
Study shows potential disease treatment in
newborns via drug delivery to amniotic fluid
6 October 2016
that holds the embryo. The procedure, performed in
mice, resulted in targeted alteration in gene
expression for up to a month after birth in some
tissue.
"A major barrier to the development of treatments
for congenital disorders is the risk to the developing
fetus that interventions may pose," said Michelle
Hastings, PhD, associate professor of cell biology
and anatomy, who led the RFU team. "Our
demonstration that this promising type of
therapeutic can be delivered to the amniotic cavity
is an important advance for fetal treatment of
disease."
The study is the first demonstration of ASO
embryonic transfer with amniotic fluid
administration, or non-surgical insertion of ASOs
into the developing fetus—a key step toward broad
application of this powerful gene therapy approach
in humans.
This is a schematic representation of transuterine
microinjection into the amniotic cavity surrounding the
E13 embryo. The microinjection pipette (blue) traverses
the uterus (red), the yolk sac cavity (ysc), the visceral
"This could be really useful in the future to treat all
yolk sac (vys, black), the exocoelomic cavity (ec) and
types of genetic diseases," said study co-author
finally the amnion (green) en route to the amniotic cavity
Lingyan Wang, Ph.D., a researcher with the
(ac). Credit: Rosalind Franklin University
Oregon Hearing Research Center at OHSU.
A breakthrough study by research teams at
Rosalind Franklin University of Medicine and
Science and Oregon Health & Science University
offers promise for therapeutic management of
congenital diseases in utero using designer
nucleotide sequences that can simply be injected
into the fluid surrounding the developing fetus to
potentially treat disabling-to-lethal genetic defects.
Congenital disease, estimated to cause the death
of ~300,000 infants within the first month of life
each year across the globe also causes childhood
illness and long-term disability. Prenatal screening
techniques now make early diagnosis possible,
presenting the opportunity to intervene in disease
processes before birth.
"The best way to treat a disease that we know will
emerge at birth is to deliver a therapy in utero to the
developing fetus before irreparable damage
occurs," said co-author John Brigande, Ph.D., a
principal investigator in the Oregon Hearing
Research Center.
Recently published in the journal Nucleic Acids
Research, the study shows that antisense
oligonucleotides (ASOs), short strands of
engineered nucleic acid that are designed to bind
to a specific gene-derived sequence, can be safely
The combination of a potentially low-risk delivery
injected into the amniotic cavity—the fluid-filled sac
approach with the promising antisense drug
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platform, which, in theory, can alter any diseaseassociated aberrant gene expression by simply
designing the sequence of the injectable molecule
to match the target gene, is an exciting
breakthrough, though more work needs to be done
to improve the efficiency of drug uptake and
distribution to specific tissues.
"We predict that fetal ASO pharmacotherapy has
the potential to safely enable therapeutic strategies
for the treatment of fetal and congenital genetic
disease," the authors wrote.
More information: Frederic F. Depreux et al,
Antisense oligonucleotides delivered to the
amniotic cavitymodulate gene expression in the
postnatal mouse, Nucleic Acids Research (2016).
DOI: 10.1093/nar/gkw867
Provided by Rosalind Franklin University of
Medicine and Science
APA citation: Study shows potential disease treatment in newborns via drug delivery to amniotic fluid
(2016, October 6) retrieved 2 May 2017 from https://medicalxpress.com/news/2016-10-potential-diseasetreatment-newborns-drug.html
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