Literature DB >> 10713568

Comparative study of the apical ganglion in planktotrophic caenogastropod larvae: ultrastructure and immunoreactivity to serotonin.

L R Page1, S C Parries.   

Abstract

Previous research suggests that a major role of the apical ganglion (also called the apical or cephalic sensory organ) in gastropod larvae is detection and integration of sensory information and relay of motor signals to effectors in the velum. However, the relative impact of ancestry versus velum size and life history on characteristics of the apical ganglion is unresolved. We address this issue by contributing data on the apical ganglion and overlying epidermis in planktotrophic larvae of four caenogastropod species (Euspira [Polinices] lewisii, Lacuna vincta, Trichotropis cancellata, and Amphissa versicolor) derived from light microscopy, scanning and transmission electron microscopy, and immunohistochemical localization of serotonin-like antigenicity. Ultrastructure of the apical ganglion is similar in these caenogastropods, and the basic plan corresponds to previous descriptions of the apical ganglion in planktotrophic opisthobranch larvae (subgroup of Heterobranchia). The only identified structural feature that is unique to all these caenogastropods, relative to opisthobranchs, is modified ciliary axonemes for the ampullary cells, a distinctive type of sensory neuron. Like opisthobranch larvae, caenogastropod larvae have serotonin-immunoreactive neurons within the apical ganglion; the number ranges from three to six, but a lateral pair of serotonergic, nonsensory neurons is common to all species. The pattern of serotonergic neurons in E. lewisii, which develops large, subdivided velar lobes, is the same as that of opisthobranch larvae, which have a relatively small, unelaborated velum. These and other data suggest that common ancestry is a major determinant of overall structural design for the apical ganglion in caenogastropods and heterobranchs, which are sister groups within the Gastropoda. Velum size and life history strategy may account for some, but not all, cases of interspecific differences in the serotonergic component. Copyright 2000 Wiley-Liss, Inc.

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Year:  2000        PMID: 10713568     DOI: 10.1002/(sici)1096-9861(20000320)418:4<383::aid-cne2>3.0.co;2-b

Source DB:  PubMed          Journal:  J Comp Neurol        ISSN: 0021-9967            Impact factor:   3.215


  14 in total

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