Tammy A. Maldonado

Distribution of β-amyloid and amyloid precursor protein in the brain of spawning (senescent) salmon: a natural, brain-aging model

Brain amyloid precursor protein (APP), a normal constituent of neurons, glial cells and cerebrospinal fluid, has several proposed functions (e.g., in neuronal growth and survival). It appears, however, that altered processing of APP is an initial or downstream step in the neuropathology of brain aging, Alzheimers disease (AD), and Downs syndrome (DS). Some studies suggest that proteolytic cleavage of APP, producing beta-amyloid (Abeta(1-42)), could have neurotoxic or neuroprotective effects. In this study, we utilized antibodies to human APP(695) and Abeta(1-42,) and Congo red staining, to search for amyloid deposition in the brain of semelparous spawning kokanee salmon (Oncorhynchus nerka kennerlyi). Intracellular APP(695) immunoreactivity (APP-ir) was observed in brain regions involved in gustation (glomerulosus complex), olfaction (putative hippocampus, olfactory bulb), vision (optic tectum), the stress response (nucleus preopticus and nucleus lateralis tuberis), reproductive behavior (nucleus preopticus magnocellularis, nucleus preopticus periventricularis, ventral telencephalon), and coordination (cerebellum). Intra- and extra-neuronal Abeta(1-42) immunoreactivity (Abeta-ir) were present in all APP-ir regions except the nucleus lateralis tuberis and Purkinje cells of the cerebellum (coordination). Thus, the relationship between APP and Abeta deposition during brain aging could shed light on the processing of APP into Abeta, neurodegeneration, and possible protection of neurons that are functioning in spawning but senescent salmon. Pacific salmon, with their predictable and synchronized life history, could provide research options not available with the existing models for studies of brain aging and amyloidosis.

Some aspects of hepatic function in feral brown trout, Salmo trutta, living in metal contaminated water

Brown trout, Salmo trutta, exposed to heavy metals (mainly Cd and Zn) for at least 2 years in the Eagle River, Colorado, were examined for liver size and activity of the growth-promoting enzyme, ornithine decarboxylase (ODC) and compared to trout living in an uncontaminated site. Liver-somatic index (LSI) was greater for trout living in the uncontaminated site with the LSI of females being significantly greater than that of males. The LSI for females at the uncontaminated site was greater than that of females at the contaminated site, but males were not different statistically. ODC activity in the livers of both males and females was lower at the contaminated site. However, males and females did not differ with respect to ODC activity. These data suggest that chronic exposure to heavy metals may have important implications for growth and reproduction and possibly survival. The activity of ODC in liver might serve as a useful biomarker when assessing chronic toxicity of metals to naturally reproducing fish populations.

Localization of gonadotropin-releasing hormone in the central nervous system and a peripheral chemosensory organ of Aplysia californica

Gonadotropin-releasing hormone (GnRH) is a neurohormone crucial for the regulation of reproductive and neural functions in vertebrates. Recent discoveries of GnRH immunoreactivity (IR) in a number of invertebrates raised the possibility that GnRH may be an ancient molecule that had arisen before the emergence of Phylum Chordata. We previously demonstrated the presence of a GnRH IR similar to the mammalian (m) and tunicate I (tI) forms of GnRH in the hemolymph and ovotestis of an opisthobranch mollusk, Aplysia californica; however, the presence of GnRH in the central nervous system (CNS) of A. californica could not be detected with the available antisera against various forms of chordate GnRH. In the present study, we performed immunohistochemistry (IHC) to localize the presence of GnRH in the CNS and a peripheral chemosensory organ, the osphradium, of A. californica. A newly generated antiserum against tI-GnRH revealed the strong expression of GnRH IR in neurons of all CNS ganglia. A notable asymmetry in immunostaining was detected in the left and right abdominal hemiganglia. The CNS is rich in tI-GnRH immunoreactive neurons but lacks mGnRH IR, whereas the osphradium contains abundant mGnRH immunoreactive neurons but lacks tI-GnRH IR. The extract of CNS failed to stimulate the release of LH from mouse pituitary, demonstrating that the A. californica GnRH IR is structurally different from what is required to bind and activate mammalian GnRH receptor. Together, these results indicate the presence of at least two distinct GnRH systems in A. californica. The presence of GnRH in the osphradium is consistent with the long-standing anatomical relationship between GnRH and the chemosensory system observed in vertebrates.