A phylogeographical perspective on the ex situ conservation of Aylacostoma (Thiaridae,Gastropoda) from the High Paraná River (Argentina–Paraguay)

Aylacostoma Spix, 1827, contains species that are the subject of focused conservation efforts under the auspices of the ‘Aylacostoma Project’, the only ex situ conservation programme for freshwater gastropods in South America. Two species from the High Paraná River (Argentina–Paraguay) are included in this programme (Aylacostoma chloroticum Hylton Scott, 1954 and Aylacostoma brunneum Vogler & Peso, 2014), as their habitats have disappeared as a consequence of the filling of the Yacyretá Reservoir in the 1990s. At present, A. chloroticum is restricted to only one known wild population in a small and fragile habitat, and wild populations of A. brunneum are presumed to have gone extinct. We used partial sequences of the cytochrome oxidase subunit I gene to provide the first phylogeographical perspective on these species from a limited dataset containing representatives of several wild populations that are successfully being bred in captivity. We found low genetic diversity and two haplotypes in A. chloroticum, and absence of variation with one haplotype in A. brunneum. The reservoir's entry zone was identified to be of great interest for conservation, and is where we suggest re‐introductions and translocations should be targeted, to preserve the future evolutionary potential of the extant diversity. © 2015 The Linnean Society of London     

Personality and fitness consequences of flight initiation distance and mating behavior in subdominant male reindeer (Rangifer tarandus)

Animal personality has been studied extensively in recent years, yet multidimensionality in tendencies of risk‐related behavior, and the role of such consistency from a mating tactics perspective, is yet to be investigated. We used a semi‐domesticated herd of reindeer (Rangifer tarandus) to examine individual subdominant male propensity to risk mating attempts on guarded females, as well as flight initiation distance (FID), within the personality paradigm to elucidate potential fitness consequences of consistency from an adaptive perspective. Data were collected at the Kutuharju Reindeer Research Station in Kaamanen, Finland, where measures of personality were generated using field observation data based on the relative frequency of dominant male–subdominant male agonistic interactions over 4 years and subdominant males' FID measured over 1 year. Individual propensity for transient mating attempts was not significantly repeatable and did not significantly predict reproductive success or somatic cost during the mating season. Individuals varied consistently in FID, and although repeatable, FID was not related to reproductive success or somatic cost. Proximate state‐dependent or social mechanisms may be driving decision‐making with respect to mating effort, whereas consistent between‐individual differences in FID may be maintained by mechanisms unrelated to life‐history trade‐offs involving productivity.     

Structure-activity relationships of pyrrole based S-nitrosoglutathione reductase inhibitors: pyrrole regioisomers and propionic acid replacement

S-Nitrosoglutathione reductase (GSNOR) is a member of the alcohol dehydrogenase family (ADH) that regulates the levels of S-nitrosothiols (SNOs) through catabolism of S-nitrosoglutathione (GSNO). GSNO and SNOs are implicated in the pathogenesis of many diseases including those in respiratory, cardiovascular, and gastrointestinal systems. The pyrrole based N6022 was recently identified as a potent, selective, reversible, and efficacious GSNOR inhibitor which is currently undergoing clinical development. We describe here the synthesis and structure-activity relationships (SAR) of novel pyrrole based analogues of N6022 focusing on scaffold modification and propionic acid replacement. We identified equally potent and novel GSNOR inhibitors having pyrrole regioisomers as scaffolds using a structure based approach.     

Assessment of cues potentially mediating host selection of Leptoglossus occidentalis on Pinus contorta

1. Leptoglossus occidentalis causes significant damage in conifer seed orchards. Host selection by L. occidentalis is not completely understood. Earlier research has demonstrated a preference for certain clones of Pinus contorta, indicating that L. occidentalis responds to chemical or physical cues.
2. The present study aimed to test whether L. occidentalis shows clonal preference across years, and to examine whether the host cues responsible for this could be identified.
3. Surveys were conducted in a lodgepole pine seed orchard in British Columbia in 2008 and 2009. Clones were ranked based on the proportion of their ramets on which L. occidentalis was observed. Ramets were divided into three classes: (i) preferred clones with seed bugs; (ii) preferred clones without seed bugs; and (iii) nonpreferred clones with zero or very low numbers of seed bugs. From each clone, we measured infrared radiation emitted from cones, cone monoterpenes, cone size and numbers of cones per tree.
4. Clone preference was consistent between 2008 and 2009. Clone preference classes differed significantly in α‐pinene and δ‐3 carene and limonene.
5. Leptoglossus occidentalis was found more frequently on clones with cones of greater diameter and weight.
6. Infrared radiation did not differ between clone preference classes, indicating that it is not used in host acceptance.

     

Late‐life rapamycin treatment reverses age‐related heart dysfunction

Rapamycin has been shown to extend lifespan in numerous model organisms including mice, with the most dramatic longevity effects reported in females. However, little is known about the functional ramifications of this longevity‐enhancing paradigm in mammalian tissues. We treated 24‐month‐old female C57BL/6J mice with rapamycin for 3 months and determined health outcomes via a variety of noninvasive measures of cardiovascular, skeletal, and metabolic health for individual mice. We determined that while rapamycin has mild transient metabolic effects, there are significant benefits to late‐life cardiovascular function with a reversal or attenuation of age‐related changes in the heart. RNA‐seq analysis of cardiac tissue after treatment indicated inflammatory, metabolic, and antihypertrophic expression changes in cardiac tissue as potential mechanisms mediating the functional improvement. Rapamycin treatment also resulted in beneficial behavioral, skeletal, and motor changes in these mice compared with those fed a control diet. From these findings, we propose that late‐life rapamycin therapy not only extends the lifespan of mammals, but also confers functional benefits to a number of tissues and mechanistically implicates an improvement in contractile function and antihypertrophic signaling in the aged heart with a reduction in age‐related inflammation.     

Two frameshift mutations in the cystic fibrosis gene

Cystic fibrosis (CF) is a recessive disease caused by mutations in the CF transmembrane conductance regulator (CFTR) gene. We have identified in exon 7 two frameshift mutations, one caused by a two-nucleotide insertion and the other caused by a one-nucleotide deletion; these mutations--CF1154insTC and CF1213delT, respectively, are predicted to shift the reading frame of the protein and to introduce UAA(ochre) termination codons at residues 369 and 368.     

Directed differentiation of dendritic cells from mouse embryonic stem cells

Dendritic cells (DCs) are uniquely capable of presenting antigen to naive T cells, either eliciting immunity [1] or ensuring self-tolerance [2]. This property identifies DCs as potential candidates for enhancing responses to foreign [3] and tumour antigens [4], and as targets for immune intervention in the treatment of autoimmunity and allograft rejection [1]. Realisation of their therapeutic potential would be greatly facilitated by a fuller understanding of the function of DC-specific genes, a goal that has frequently proven elusive because of the paucity of stable lines of DCs that retain their unique properties, and the inherent resistance of primary DCs to genetic modification. Protocols for the genetic manipulation of embryonic stem (ES) cells are, by contrast, well established [5], as is their capacity to differentiate into a wide variety of cell types in vitro, including many of hematopoietic origin [6]. Here, we report the establishment, from mouse ES cells, of long-term cultures of immature DCs that share many characteristics with macrophages, but acquire, upon maturation, the allostimulatory capacity and surface phenotype of classical DCs, including expression of CD11c, major histocompatibility complex (MHC) class II and co-stimulatory molecules. This novel source should prove valuable for the generation of primary, untransformed DCs in which candidate genes have been overexpressed or functionally ablated, while providing insights into the earliest stages of DC ontogeny.     

Dolichol alters dynamic and static properties of mouse synaptosomal plasma membranes

Dolichols are isoprenologues that are found in almost all tissues and whose biochemical function, aside from dolichol phosphate precursors, is not known. In addition, an understanding of the organizational and dynamic properties of dolichols in biological membranes has not been forthcoming. The purpose of the experiments reported here were to examine the effects of dolichol on the physical properties of mouse synaptic plasma membranes (SPM). Differential polarized phase fluorometry indicated that dolichol both fluidized and rigidified SPM. Membrane areas detected by diphenylhexatriene and trans-parinaric acid were selectively fluidized and rigidified, respectively. It also was found that the spin label, 5-doxyl stearic acid indicated that dolichol reduced membrane fluidity. These results report for the first time a structural effect of dolichol on a biological membrane.