Several microsatellite-expansion diseases are char�acterized by the accumulation of RNA foci and RAN
proteins, raising the possibility of a mechanistic
connection. We explored this question using myoto�nic dystrophy type 2, a multisystemic disease thought
to be primarily caused by RNA gain-of-function
effects. We demonstrate that the DM2 CCTG,CAGG
expansion expresses sense and antisense tetrapep�tide poly-(LPAC) and poly-(QAGR) RAN proteins,
respectively. In DM2 autopsy brains, LPAC is found
in neurons, astrocytes, and glia in gray matter, and
antisense QAGR proteins accumulate within white
matter. LPAC and QAGR proteins are toxic to cells in�dependent of RNA gain of function. RNA foci and nu�clear sequestratio... More
Several microsatellite-expansion diseases are char�acterized by the accumulation of RNA foci and RAN
proteins, raising the possibility of a mechanistic
connection. We explored this question using myoto�nic dystrophy type 2, a multisystemic disease thought
to be primarily caused by RNA gain-of-function
effects. We demonstrate that the DM2 CCTG,CAGG
expansion expresses sense and antisense tetrapep�tide poly-(LPAC) and poly-(QAGR) RAN proteins,
respectively. In DM2 autopsy brains, LPAC is found
in neurons, astrocytes, and glia in gray matter, and
antisense QAGR proteins accumulate within white
matter. LPAC and QAGR proteins are toxic to cells in�dependent of RNA gain of function. RNA foci and nu�clear sequestration of CCUG transcripts by MBNL1 is
inversely correlated with LPAC expression. These
data suggest a model that involves nuclear retention
of expansion RNAs by RNA-binding proteins (RBPs)
and an acute phase in which expansion RNAs exceed
RBP sequestration capacity, are exported to the cyto�plasm, and undergo RAN translation
