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Vol. 9, Issue 5, 1007-1023, May 1998

and
*Cold Spring Harbor Laboratory, Cold Spring Harbor, New York 11724;
and
Antisense oligonucleotides are powerful tools for the in vivo
regulation of gene expression. We have characterized the intracellular distribution of fluorescently tagged phosphorothioate
oligodeoxynucleotides (PS-ONs) at high resolution under conditions in
which PS-ONs have the potential to display antisense activity. Under
these conditions PS-ONs predominantly localized to the cell nucleus
where they accumulated in 20-30 bright spherical foci designated
phosphorothioate bodies (PS bodies), which were set against a diffuse
nucleoplasmic population excluding nucleoli. PS bodies are nuclear
structures that formed in cells after PS-ON delivery by transfection
agents or microinjection but were observed irrespectively of antisense activity or sequence. Ultrastructurally, PS bodies corresponded to
electron-dense structures of 150-300 nm diameter and resembled nuclear
bodies that were found with lower frequency in cells lacking PS-ONs.
The environment of a living cell was required for the de novo formation
of PS bodies, which occurred within minutes after the introduction of
PS-ONs. PS bodies were stable entities that underwent noticeable
reorganization only during mitosis. Upon exit from mitosis, PS bodies
were assembled de novo from diffuse PS-ON pools in the daughter nuclei.
In situ fractionation demonstrated an association of PS-ONs with the
nuclear matrix. Taken together, our data provide evidence for the
formation of a nuclear body in cells after introduction of
phosphorothioate oligodeoxynucleotides.
ISIS Pharmaceuticals, Carlsbad, California 92008
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