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Galanin Expression in the Mouse Major Pelvic Ganglia During Explant Culture and Following Cavernous Nerve Transection

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Abstract

Autonomic neurons commonly respond to injury/axotomy with an increased expression of neuropeptides including galanin and pituitary adenylyl cyclase-activating polypeptide (PACAP). The increased peptide expression may enhance neuronal survival and axonal regeneration. Using quantitative (Q) PCR and immunocytochemistry, the present study tested whether galanin expression increased in male mouse major pelvic ganglia (MPG) neurons in response to injury. Galanin transcript expression increased significantly in MPG neurons following 72 h in explant culture and 72 h after unilateral transection of the cavernous nerve. Under both conditions, the increase in galanin transcript levels was greater than the increase in PACAP transcript levels. In control MPG, galanin-IR nerve fibers formed pericellular arrangements around MPG neurons although few galanin-IR cells were evident and many of the galanin-IR cells may be small intensely fluorescent (SIF) cells. In 3-day-cultured MPGs, many more galanin-IR cells and nerve fibers were noted. The increased galanin expression was most apparent in neurons that were also immunoreactive for neuronal nitric oxide synthase, rather than tyrosine hydroxylase. Some explant-cultured MPG neurons exhibited immunoreactivity to galanin and PACAP. As reported previously for PACAP, there is an injury-induced increase in MPG galanin expression, which occurs preferentially in the parasympathetic postganglionic neurons.

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Acknowledgments

The study was supported in part by NIH grants R01 DK060481 and R01 DK051369 to MAV and NIH grants P20 RR16435, P30 RR032135, and P30 GM103498 to RLP. We thank Dr. Jan Fahrenkrug for kindly providing the PACAP antiserum.

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Correspondence to Rodney L. Parsons.

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Girard, B.M., Galli, J.R., Vizzard, M.A. et al. Galanin Expression in the Mouse Major Pelvic Ganglia During Explant Culture and Following Cavernous Nerve Transection. J Mol Neurosci 48, 713–720 (2012). https://doi.org/10.1007/s12031-012-9810-9

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  • DOI: https://doi.org/10.1007/s12031-012-9810-9

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