Abstract

“Rods and rings” (RR) and loukoumasomes are similarly shaped, subcellular macromolecular structures with as yet unknown function. RR, so named because of their shape, are formed in response to inhibition in the GTP or CTP synthetic pathways and are highly enriched in the two key enzymes of the nucleotide synthetic pathway. Loukoumasomes also occur as linear and toroidal bodies and were initially inferred to be the same as RR, largely due to their shared shape and size and the fact that it was unclear if they shared the same subcomponents. In human retinoblastoma tissue and cells we have observed toroidal, perinuclear, macromolecular structures of similar size and antigenicity to those previously reported in neurons (neuronal-loukoumasomes). To further characterize the subcomponents of the retinal-loukoumasomes, confocal analysis following immunocytochemical staining for alpha-tubulin, beta-III tubulin and detyrosinated tubulin was performed. These studies indicate that retinal-loukoumasomes are enriched for beta-III tubulin and other tubulins associated with microtubules. Immunofluorescence together with the in situ proximity ligation assay (PLA), confirmed that beta-III tubulin colocalized with detyrosinated tubulin within loukoumasomes. Our results indicate that these tissues contain only loukoumasomes because these macromolecular structures are immunoreactive with an anti-tubulin antibody but are not recognized by the prototype anti-RR/inosine monophosphate dehydrogenase (IMPDH) antibody (It2006). To further compare the RR and retinal-loukoumasomes, retinoblastoma cells were exposed to the IMPDH-inhibitor ribavirin, a drug known to induce the formation of RR. In contrast to RR, the production of retinal-loukoumasomes was unaffected. Coimmunostaining of Y79 cells for beta-III tubulin and IMPDH indicate that these cells, when treated with ribavirin, can contain both retinal-loukoumasomes and RR and that these structures are antigenically distinct. Subcellular fractionation studies indicate that ribavirin increased the RR subcomponent, IMPDH, in the nuclear fraction of Y79 cells from 21.3 ± 5.8% (0 mM ribavirin) to 122.8 ± 7.9% (1 mM ribavirin) while the subcellular localization of the retinal-loukoumasome subcomponent tubulin went unaltered. Further characterization of retinal-loukoumasomes in retinoblastoma cells reveals that they are intimately associated with lamin folds within the nuclear envelope. Using immunofluorescence and the in situ PLA in this cell type, we have observed colocalization of beta-III tubulin with MAP2. As MAP2 is a microtubule-associated protein implicated in microtubule crosslinking, this supports a role for microtubule crosslinkers in the formation of retinal-loukoumasomes. Together, these results suggest that loukoumasomes and RR are distinct subcellular macromolecular structures, formed by different cellular processes and that there are other loukoumasome-like structures within retinal tissues and cells.

Highlights

  • Rods and rings (RR), first described in 2005 [1], are subcellular structures that occur as toroidal bodies and rods

  • The toroids we found within retinoblastoma tissue and cells were similar in size and shape to the toroids found in rat sympathetic neurons

  • We identified RR and loukoumasomes as distinct toroidal and spherical structures within human retinoblastoma tissue and dissociated human retinoblastoma cells

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Summary

Introduction

Rods and rings (RR), first described in 2005 [1], are subcellular structures that occur as toroidal bodies and rods (for recent reviews see [2, 3]). Structures, thought to be intermediate between rods and rings, with a “sewing pin” and “figure eight” shape, have been reported [2] These structures are found predominantly in the cytoplasm, smaller versions have been found in the nucleus [5] (for review see [3]). Autoantibodies to IMPDH in RR have been found in hepatitis-C positive patients who were taking ribavirin and interferon-alpha; the formation of RR appears to be independent of infection with the hepatitis C virus [6, 20, 23]. Both ribavirin and interferon-alpha were subsequently tested in vitro to determine their effect on cultured cells; the IMPDH inhibitor ribavirin induced formation of RR in >95% of cultured cells while interferon-alpha had no effect [4, 6]

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