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Published September 7, 2006 | Supplemental Material
Journal Article Open

The Prototoxin lynx1 Acts on Nicotinic Acetylcholine Receptors to Balance Neuronal Activity and Survival In Vivo

Miwa, Julie M.
Stevens, Tanya R.
King, Sarah L.
Caldarone, Barbara J.
Ibanez-Tallon, Ines
Xiao, Cheng ORCID icon
Fitzsimonds, Reiko Maki
Pavlides, Constantine
Lester, Henry A. ORCID icon
Picciotto, Marina R.
Heintz, Nathaniel

Abstract

Nicotinic acetylcholine receptors (nAChRs) affect a wide array of biological processes, including learning and memory, attention, and addiction. lynx1, the founding member of a family of mammalian prototoxins, modulates nAChR function in vitro by altering agonist sensitivity and desensitization kinetics. Here we demonstrate, through the generation of lynx1 null mutant mice, that lynx1 modulates nAChR signaling in vivo. Its loss decreases the EC₅₀ for nicotine by ∼10-fold, decreases receptor desensitization, elevates intracellular calcium levels in response to nicotine, and enhances synaptic efficacy. lynx1 null mutant mice exhibit enhanced performance in specific tests of learning and memory. Consistent with reports that mutations resulting in hyperactivation of nAChRs can lead to neurodegeneration, aging lynx1 null mutant mice exhibit a vacuolating degeneration that is exacerbated by nicotine and ameliorated by null mutations in nAChRs. We conclude that lynx1 functions as an allosteric modulator of nAChR function in vivo, balancing neuronal activity and survival in the CNS.

Additional Information

© 2006 Elsevier Inc. Received 21 December 2004, Revised 21 October 2005, Accepted 19 July 2006, Available online 6 September 2006. We wish to thank A.L. Beaudet for generously providing the α7 and β2 nAChR mutant mice used in these experiments. Special thanks to Dr. Andreas Walz, Dr. S. Selesnick, and Dr. P. Gutin. For helpful scientific discussions and/or technical support, thanks to C. Fletcher, R.A. Lester, A.B. Tekinay, R. Nashmi, A. Tapper, R. Pantoja, F. Moss, and B. Cohen and other members of HAL lab; B. Switzer of NSA, A. Kolar, S. Krueger, and A. Aslantas. Support for M.R.P., S.L.K., B.J.C., and T.R.S.: DA00436, DA15241, and AA15632; for J.M.M., NIH CA09673; for N.H., J.M.M., and I.I.-T., HHMI and NIH NIH R21 NS047751; for H.A.L. and C.X., DA-17279 and CA Tobacco-Related Disease Research Project.

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Identifiers Funding Dates
Created:
August 22, 2023
Modified:
October 20, 2023