A histological description of gonadal development and sex differentiation in the coho salmon (Oncorhynchus kisutch) for both untreated and oestradiol immersed fry

Gonadal development is described in detail for coho salmon ( Oncorhynchus kisutch ) between hatching and 1000 degree-days, post-hatch, to aid sex reversal research. Germ cell morphology and sequence, vascular and reproductive duct development, and gross characteristics of the gonads are presented. Sex differentiation occurs by 380 degree-days, post-hatch (800 degree-days, post-fertilization) and is direct to male and female. Oocytes proliferate rapidly after differentiation while the testes enter a period of quiescence. Fry immersed for short durations in oestradiol (200 μg ⁻¹) are also examined. Hormone immersion advanced sex differentiation by 70 degree-days. The immersions were applied early, at 20 and 90 degree-days, post-hatch, yet still altered the sex ratio and timing of differentiation. Definitive germ cells, which are abundant during this period, may be the type most receptive to steroid treatment.     

Fork-Remodeling Helicase Rad5 Preferentially Reverses Replication Forks with Gaps in the Leading Strand

DNA damage bypass pathways promote the replication of damaged DNA when replication forks stall at sites of DNA damage. Template switching is a DNA damage bypass pathway in which fork-reversal helicases convert stalled replication forks into four-way DNA junctions called chicken foot intermediates, which are subsequently extended by replicative DNA polymerases. In yeast, fork-reversal is carried out by the Rad5 helicase using an unknown mechanism. To better understand the mechanism of Rad5 and its specificity for different fork DNA substrates, we used a FRET-based assay to observe fork reversal in real time. We examined the ability of Rad5 to bind and catalyze the reversal of various fork DNA substrates in the presence of short gaps in the leading or lagging strand as well as in the presence or absence of RPA and RNA primers in the lagging strand. We found that Rad5 preferentially reverses fork DNA substrates with short gaps (10 to 30 nt.) in the leading strand. Thus, Rad5 preferentially reverses fork DNA substrates that form chicken foot intermediates with 5′ overhangs that can be extended by replicative DNA polymerases during the subsequent steps of template switching.     

Quantitative trait loci for body growth and sex determination in the hermaphrodite teleost fish Sparus aurata L.

Gilthead sea bream (Sparus aurata L.) is an important marine fish in Mediterranean aquaculture. Sex determination by age and/or body weight is a critical life‐history trait, the genetic basis for which is largely unknown in this sequential hermaphrodite species. Herein, we performed a partial genome scan to map quantitative trait loci (QTL) affecting body weight and sex using 74 informative microsatellite markers from 10 paternal half‐sib families to construct nine linkage groups (LG). In total, four growth‐related QTL (two chromosome‐wide and two genome‐wide) and six QTL related to sex determination (three pairs in three different LGs) were detected (two chromosome‐wide and one genome‐wide). The proportion of phenotypic variation explained by the body‐weight QTL ranged from 9.3% to 17.2%, showing their potential for use in marker‐assisted selection. The results obtained offer solid ground to investigate the structure and function of the genomic regions involved in the mechanisms of sex reversal.     

Differential roles of CaMKII isoforms in phase separation with NMDA receptors and in synaptic plasticity

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The Case for Intervention Bias in the Practice of Medicine

Bias is an inclination to present or hold a partial perspective at the expense of possibly equal or more valid alternatives. In this paper, we present a series of conditional arguments to prove that intervention bias exists in the practice of medicine. We then explore its potential causes, consequences, and criticisms. We use the term to describe the bias on the part of physicians and the medical community to intervene, whether it is with drugs, diagnostic tests, non-invasive procedures, or surgeries, when not intervening would be a reasonable alternative. The recognition of intervention bias in medicine is critically important given today’s emphasis on providing high-value care and reducing unnecessary and potentially harmful interventions.     

New phenstatin–fatty acid conjugates: Synthesis and evaluation

New phenstatin–fatty acid conjugates have been synthesized and tested against the KB-3-1, H460, MCF-7 and HEK293 cell lines, with an increase in anti-proliferative activity being observed at the micro-molar level paralleling an increase in un-saturation in the fatty acid component.     

The gravitropic set-point angle (GSA): the identification of an important developmentally controlled variable governing plant architecture*

The angle at which an organ is maintained by gravit-ropism is characteristic of the organ, its developmental state and the prevailing environmental conditions. We propose that this angle be called the gravitropic set-point angle (GSA), defined as the angle with respect to the gravity vector (with a vertically downward orientation being 0°) at which an organ is maintained as a consequence of gravitropism. Studies of the gravitropic behaviour of organs from trailing plants show that the GSA is subject to developmental regulation. Depending on the developmental age and prevailing environmental conditions, the GSA of an organ can he set at any value between 0° and 180° The previously reported reversal of the sign of the gravitropic response in such organs, whether this is brought about developmentally or induced by light, represents the change from one common extreme (GSA = 180°, conventionally referred to as negative orthogravitropism) to another (GSA = 0°, or positive orthogravitropism). The concept of a variable gravitropic set-point offers a more unified view of all forms of gravitropic behaviour than has been advanced previously, and places a new constraint on models of gravitropism. Current models of gravitropism appear to be unable to explain either the ability of organs to change their orientation with respect to gravity as they develop, or the re-orientation that can be observed when some organs are exposed to new environmental conditions.     

Heritable variation in locomotion,reward sensitivity and impulsive behaviors in a genetically diverse inbred mouse panel

Drugs of abuse, including alcohol and stimulants like cocaine, produce effects that are subject to individual variability, and genetic variation accounts for at least a portion of those differences. Notably, research in both animal models and human subjects point toward reward sensitivity and impulsivity as being trait characteristics that predict relatively greater positive subjective responses to stimulant drugs. Here we describe use of the eight collaborative cross (CC) founder strains and 38 (reversal learning) or 10 (all other tests) CC strains to examine the heritability of reward sensitivity and impulsivity traits, as well as genetic correlations between these measures and existing addiction-related phenotypes. Strains were all tested for activity in an open field and reward sensitivity (intake of chocolate BOOST®). Mice were then divided into two counterbalanced groups and underwent reversal learning (impulsive action and waiting impulsivity) or delay discounting (impulsive choice). CC and founder mice show significant heritability for impulsive action, impulsive choice, waiting impulsivity, locomotor activity, and reward sensitivity, with each impulsive phenotype determined to be non-correlating, independent traits. This research was conducted within the broader, inter-laboratory effort of the Center for Systems Neurogenetics of Addiction (CSNA) to characterize CC and DO mice for multiple, cocaine abuse related traits. These data will facilitate the discovery of genetic correlations between predictive traits, which will then guide discovery of genes and genetic variants that contribute to addictive behaviors.     

The Relationship Between Adhesion Molecules and Neuronal Plasticity

1. It is presently widely assumed that structural reorganization of synaptic architectures subserves the functional gains that define certain neuronal plasticities.2. While target molecules thought to participate in such morphological dynamics are not well defined, growing evidence suggests a pivotal role for cell adhesion molecules.3. Herein, brief discussions are presented on (i) the history of how adhesion molecules became implicated in plasticity and memory processes, (ii) the general biology of some of the major classes of such molecules, and (iii) the future of the adhesion molecule/plasticity relationship.