Abnormal cells in the early embryo are not necessarily a sign
that a baby will be born with a birth defect such as Down's
syndrome, suggests new research from the University of Cambridge,
the Wellcome Trust Sanger Institute and the University of Leuven,
Belgium.
The scientists show that abnormal cells are eliminated and
replaced by healthy cells, repairing - and in many cases completely
fixing - the embryo.
Cambridge researchers report a mouse model of aneuploidy, where
some cells in the embryo contain an abnormal number of chromosomes.
Normally, each cell in the human embryo should contain 23 pairs of
chromosomes (22 pairs of chromosomes and one pair of sex
chromosomes), but some can carry multiple copies of chromosomes,
which can lead to developmental disorders. For example, children
born with three copies of chromosome 21 will develop Down's
syndrome.
Pregnant mothers - particular older mothers, whose offspring are
at greatest risk of developing such disorders - are offered tests
to predict the likelihood of genetic abnormalities. Between the
11th and 14th weeks of pregnancy, mothers may be offered chorionic
villus sampling (CVS), a test that involves removing and analysing
cells from the placenta. A later test, known as amniocentesis,
involves analysing cells shed by the foetus into the surrounding
amniotic fluid - this test is more accurate, but is usually carried
out during weeks 15-20 of the pregnancy, when the foetus is further
developed.
Professor Magdalena Zernicka-Goetz, the study's senior author,
was inspired to carry out the research following her own experience
when pregnant with her second child. At the time, a CVS test found
that as many as a quarter of the cells in the placenta that joined
her and her developing baby were abnormal: could the developing
baby also have abnormal cells? When Professor Zernicka-Goetz spoke
to geneticists about the potential implications, she found that
very little was understood about the fate of embryos containing
abnormal cells and about the fate of these abnormal cells within
the developing embryos.
Fortunately for Professor Zernicka-Goetz, her son, Simon, was
born healthy. She said: "Many expectant mothers have to make a
difficult choice about their pregnancy based on a test whose
results we don't fully understand. What does it mean if a quarter
of the cells from the placenta carry a genetic abnormality - how
likely is it that the child will have cells with this abnormality,
too? This is the question we wanted to answer. Given that the
average age at which women have their children is rising, this is a
question that will become increasingly important."
Professor Thierry Voet from the Wellcome Trust Sanger Institute
and the University of Leuven in Belgium, said: "In fact, abnormal
cells with numerical and/or structural anomalies of chromosomes
have been observed in as many as 80-90 per cent of human
early-stage embryos following in vitro fertilization and CVS tests
may expose some degree of these abnormalities."
Professor Zernicka-Goetz and colleagues developed a mouse model
of aneuploidy by mixing eight-cell stage mouse embryos in which the
cells were normal with embryos in which the cells were abnormal.
Abnormal mouse embryos are relatively unusual, so the team used a
molecule known as reversine to induce aneuploidy.
In embryos where the mix of normal and abnormal cells was half
and half, the researchers observed that the abnormal cells within
the embryo were killed off by 'apoptosis', or programmed cell
death, even when placental cells retained abnormalities. This
allowed the normal cells to take over, resulting in an embryo where
all the cells were healthy. When the mix of cells was three
abnormal cells to one normal cell, some of abnormal cells continued
to survive, but the ratio of normal cells increased.
Professor Zernicka-Goetz said: "The embryo has an amazing
ability to correct itself. We found that even when half of the
cells in the early-stage embryo are abnormal, the embryo can fully
repair itself. This means that even when early indications suggest
a child might have a birth defect because there are some, but
importantly not all abnormal cells in its embryonic body, this
isn't necessarily the case."
The researchers will now try to determine the exact proportion
of healthy cells needed to completely repair an embryo and the
mechanism by which the abnormal cells are eliminated.
The paper, Mouse model of chromosome mosaicism reveals lineage-specific
depletion of aneuploid cells and normal developmental
potential, is published in Nature Communications.