Abstract

Early odor preference learning in rodents occurs within a sensitive period [≤postnatal day (P)10–12], during which pups show a heightened ability to form an odor preference when a novel odor is paired with a tactile stimulation (e.g., stroking). Norepinephrine (NE) release from the locus coeruleus during stroking mediates this learning. However, in older pups, stroking loses its ability to induce learning. The cellular and circuitry mechanisms underpinning the sensitive period for odor preference learning is not well understood. We first established the sensitive period learning model in mice – odor paired with stroking induced odor preference in P8 but not P14 mice. This learning was dependent on NE-β-adrenoceptors as it was prevented by propranolol injection prior to training. We then tested whether there are developmental changes in pyramidal cell excitability and NE responsiveness in the anterior piriform cortex (aPC) in mouse pups. Although significant differences of pyramidal cell intrinsic properties were found in two age groups (P8–11 and P14+), NE at two concentrations (0.1 and 10 μM) did not alter intrinsic properties in either group. In contrast, in P8–11 pups, NE at 0.1 μM presynaptically decreased miniature IPSC and increased miniature EPSC frequencies. These effects were reversed with a higher dose of NE (10 μM), suggesting involvement of different adrenoceptor subtypes. In P14+ pups, NE at higher doses (1 and 10 μM) acted both pre- and postsynaptically to promote inhibition. These results suggest that enhanced synaptic excitation and reduced inhibition by NE in the aPC network may underlie the sensitive period.

Highlights

  • Critical periods of early postnatal life for neural circuitry development and plasticity occur in several sensory systems (Hensch, 2004)

  • NE is released from the locus coeruleus (LC) following tactile stimulation (Nakamura et al, 1987; Nakamura and Sakaguchi, 1990; Rangel and Leon, 1995) and pharmacological blocking of either α- or β-adrenoceptors in the olfactory bulb (OB; Sullivan et al, 2000b; Shakhawat et al, 2012), or the anterior piriform cortex, prevents early odor preference learning in rat pups

  • We tested whether the early odor preference learning in P8 mice was dependent on NE β-adrenoceptors as in rat pups (Sullivan et al, 2000b)

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Summary

Introduction

Critical periods of early postnatal life for neural circuitry development and plasticity occur in several sensory systems (Hensch, 2004). Odor preference learning can have life-long influences, for example, affecting sexual preference in adult rats (Fillion and Blass, 1986). Such preference learning is only acquired during the first one and a half weeks of life; beyond this period, stroking loses its effectiveness as a UCS (Woo and Leon, 1987) and mild shock induces odor aversion instead of preference (Camp and Rudy, 1988; Sullivan et al, 2000a; Roth et al, 2013). Odor preference learning can be acquired when a novel odor is paired with α- or β-adrenoceptor activation (Sullivan et al, 2000b; Harley et al, 2006; Morrison et al, 2013)

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