Effects of Thimerosal on NGF Signal Transduction and Cell Death in Neuroblastoma Cells

doi:10.1093/toxsci/kfi175

ToxSci Advance Access originally published online on April 20, 2005
Toxicological Sciences 2005 86(1):132-140; doi:10.1093/toxsci/kfi175

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Effects of Thimerosal on NGF Signal Transduction and Cell Death in Neuroblastoma Cells

Damani K. Parran, Angela Barker and Marion Ehrich¹

Virginia-Maryland Regional College of Veterinary Medicine, Laboratory for Neurotoxicity Studies, Virginia Tech, 1 Duckpond Drive, Blacksburg, Virginia 24061-0442

Received February 8, 2005; accepted April 13, 2005

Signaling through neurotrophic receptors is necessary for differentiationand survival of the developing nervous system. The present studyexamined the effects of the organic mercury compound thimerosalon nerve growth factor signal transduction and cell death ina human neuroblastoma cell line (SH-SY5Y cells). Following exposureto 100 ng/ml NGF and increasing concentrations of thimerosal(1 nM–10 µM), we measured the activation of TrkA,MAPK, and PKC- ${delta}$ . In controls, the activation of TrkA MAPK andPKC- ${delta}$ peaked after 5 min of exposure to NGF and then decreasedbut was still detectable at 60 min. Concurrent exposure to increasingconcentrations of thimerosal and NGF for 5 min resulted in aconcentration-dependent decrease in TrkA and MAPK phosphorylation,which was evident at 50 nM for TrkA and 100 nM for MAPK. Cellviability was assessed by the LDH assay. Following 24-h exposureto increasing concentrations of thimerosal, the EC₅₀ for celldeath in the presence or absence of NGF was 596 nM and 38.7nM, respectively. Following 48-h exposure to increasing concentrationsof thimerosal, the EC₅₀ for cell death in the presence and absenceof NGF was 105 nM and 4.35 nM, respectively. This suggests thatNGF provides protection against thimerosal cytotoxicity. Todetermine if apoptotic versus necrotic cell death was occurring,oligonucleosomal fragmented DNA was quantified by ELISA. Controllevels of fragmented DNA were similar in both the presence andabsence of NGF. With and without NGF, thimerosal caused elevatedlevels of fragmented DNA appearing at 0.01 µM (apoptosis)to decrease at concentrations >1 µM (necrosis). Thesedata demonstrate that thimerosal could alter NGF-induced signalingin neurotrophin-treated cells at concentrations lower than thoseresponsible for cell death.

Key Words: signal transduction; neurotrophin; mercury compound.

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