Breeding biology of Mountain Plovers ( Charadrius montanus ) in the Uinta Basin

The known Mountain Plover population breeding on the Myton Bench, Duchesne County, Utah, is small, composed roughly of 30 adults and young after each breeding season. Currently, its location is peripheral to the species main range. This shrub-steppe breeding habitat differs from the shortgrass prairie habitat with which this bird is historically associated. Between 1996 and 1998 we made observations at nesting sites located consistently in 2 concentrated areas surrounded by large tracts of similar habitat. Activity may be focused in these specific areas because of breeding-site fidelity; this behavior is common among most shorebirds and has been documented for the Mountain Plover in Colorado. Also, Mountain Plovers are social and tend to choose nest sites near others. Most nests in Utah were located within close proximity of mounds of white-tailed prairie dogs ( Cynomys leucurus ), and all were situated near roadways or oil well pads. Mountain Plovers were often observed with broods on these bare areas at night. We conclude that Mountain Plovers on the Myton Bench are distributed in clumped breeding colonies within large areas of apparently favorable habitat.     

The effect of moderate hemodilution with fluosol-DA or normal saline on acetaminophen disposition in the rat

Hemodilution with 40 ml/kg of Fluosol or saline reduced the acetaminophen Vd and the acetaminophen sulfate ClM at 48 or 72 h, respectively. Fluosol hemodilution increased the acetaminophen renal excretion at 24 and 72 h. But at 48 h, Fluosol hemodilution either inhibited the renal secretion of acetaminophen or enhanced its reabsorption.     

Preliminary observations of a bacteriophage infectingXenorhabdus luminescens (Enterobacteriaceae)

A bacteriophage infective toXenorhabdus luminescens, a bacterial symbiont of heterorhabditid nematodes, was recovered from insects that supported poor nematode development. Plaque tests showed the phage particles to be infective only to primary and not secondary colonies ofX. luminescens. The phage was not infective toX. nenatophilus primaries or secondaries. The bacteriophage particles ranged 80–90 nm in length, with the head ranging from 40 to 50 nm in diameter. Restriction analysis was performed on isolated bacteriophage DNA. This first report of a bacteriophage fromXenorhabdus species has pratical implications since it could be detrimental to cultures ofHeterorhabditis nematodes that are being produced throughout the world for the biological control of insects.     

Peripheral myelin protein-22 gene maps in the duplication in chromosome 17p11.2 associated with Charcot-Marie-Tooth 1A.

Charcot-Marie-Tooth disease 1A (CMT1A) is a hereditary demyelinating peripheral neuropathy, associated with a DNA duplication on chromosome 17p11.2. A related disorder in the mouse, trembler (Tr), maps to mouse chromosome 11 which has syntenic homology to human chromosome 17p. Recently, the peripheral myelin protein-22 (pmp-22) gene was identified as the likely Tr locus. We have constructed a partial yeast artificial chromosome contig spanning the CMT1A gene region and mapped the PMP-22 gene to the duplicated region. These observations further implicate PMP-22 as a candidate gene for CMT1A, and suggest that over-expression of this gene may be one mechanism that produces the CMT1A phenotype.     

New partial skeleton of Homo habilis from Olduvai Gorge, Tanzania

A new partial skeleton of an adult hominid from lower Bed I (about 1.8 Myr ago), Olduvai Gorge, is described. This specimen's craniodental anatomy indicates attribution to Homo habilis, but its postcranial anatomy, including small body size and relatively long arms, is strikingly similar to that of some early Australopithecus individuals.     

Potential carcinolytic agents. VI. New deactivated biological alkylating agents

Résumé Les auteurs ont effectué de nouvelles préparations chimiques anticancéreuses en utilisant une forme des agents alkylants déactivés du type moutarde nitrogénée quaternaire. Un mode d'action est proposé par lequel ces préparations peuvent être activées in vivo.

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Sponsored by the Cancer Chemotherapy National Service Center, National Cancer Institute, National Institutes of Health, Contract No. SA-43-ph-4360.     

Inhibition of histamine secretion from mast cells

Histamine secretion from mast cells may be inhibited by elevated intracellular levels of cyclic AMP and by several anti-allergic drugs. These compounds are claimed to act directly on the calcium-gating mechanism activated by the anaphylactic reaction, preventing influx of Ca2+ from the external environment and so blocking exocytosis. To examine this hypothesis further, we have compared here the histamine secretion induced by immunoglobulin E-directed ligands in the presence and absence of added calcium and by the ionophore A23187. Exocytosis evoked by these former agents was originally considered to be almost totally dependent on extracellular calcium but recent studies have shown otherwise. In the absence of added cation, the agents act by mobilizing membrane-bound or intracellular stores of calcium. We show that here that a variety of anti-allergic drugs are potent inhibitors in the conditions used, suggesting that alternative explanations for their action must be sought.