A man in his early 30s suddenly developed weakness in his
hands and neck, followed weeks later by burning muscle
pain—all symptoms of late-onset muscular dystrophy. His
internist ordered genetic tests to determine whether he had one
of the most common adult-onset muscular dystrophies—myotonic
dystrophy type 1 (DM1) or myotonic dystrophy type 2 (DM2). The
tests detect mutations in the DMPK and CNBP genes, the only
genes known to be associated with DM1 and DM2. While awaiting
the results of the gene tests, the internist explained that the
disease-causing mutations in these genes do not result in changes
to the coding sequence. Rather, myotonic dystrophies result
from increased, or expanded, numbers of tri- and tetranucleotide
repeats in the 3 untranslated region of the DMPK or CNBP genes.
The doctor went on to explain that the presence of RNAs with
expanded numbers of repeats leads to aberrant alternative splicing
of other mRNAs, causing widespread disruption of cellular pathways.
This discussion raises a number of interesting questions.

DM1 is characterized by a phenomenon known as genetic
anticipation where the age of onset tends to
decrease and the severity of the symptoms tend to increase
from one generation to the next due to expansion of the trinucleotide
repeats in the DMPK gene. What are the implications
of a diagnosis of DM1 in this patient with respect to his 4-yearold
son, and 2-year-old daughter?