Growing in darkness: The etiolated lupin hypocotyls

Epigeal germination of a dicot, like lupin (Lupinus albus L.), produces a seedling with a characteristic hypocotyl, which grows in darkness showing a steep growth gradient with an elongation zone just below the apex. The role of phytohormones, such as auxin and ethylene, in etiolated hypocotyl growth has been the object of our research for some time. The recent cloning and expression of three genes of influx and efflux carriers for polar auxin transport (LaAUX1, LaPIN1 and LaPIN3) reinforces a previous model proposed to explain the accumulation of auxin in the upper growth zone of the hypocotyl.Key words: auxin carriers, auxin transport gradient, etiolated hypocotyl growth, Lupinus albusMost plants show a typical axial polar and branched (dendritic) morphology to compensate for their immobility by optimally exploiting the resources available in a limited environment.From Julius von Sachs¹ to Tsvi Sachs² many plant physiologists sought to explain how the axis is maintained and what type of signals are interchanged between poles. It was demonstrated that auxins were the determining factors in maintaining the polarity in shoots and roots and a reductionistic approach leads to conclude that such polarity had to be established at the cellular level. A chemiosmotic theory was then proposed, which implied an asymmetric distribution of efflux carriers at the bottom of a cell, linked to pH gradients to maintain different undissociated/dissociated forms of auxin separated between apoplast and symplast spaces.³In recent years, the use of Arabidopsis thaliana as a plant model has given additional support to the hypothesis that polar auxin transport is restricted to certain cells and mediated by influx (AUX1 and LAX1–4 proteins) and efflux carriers (PIN1–8 proteins).^4–6 Currently, we have a good idea of the topology of Arabidopsis carrier distribution, especially in roots.^4,5 Additional (MDR/PGP)⁷ or parallel (TRH1)⁸ components of the transport system are now emerging.However, while accepting the enormous advances and contributions to plant science provided by the use of Arabidopsis thaliana, we remain true (loyal) to the particular model adopted by the Department of Plant Biology, University of Murcia (Spain) in the 1970''s: the hypocotyl of lupin seedlings cultivated in darkness. In such conditions, the organ grows heterotrophically and longer than in light.The cotyledons and meristem at the top supply nutrients and hormones in a basipetal direction.The hypocotyl is a cylindrical column, with a radial symmetry that clearly shows differentiated tissues: epidermis, cortex, vascular cylinder and pith. Its size allows surgical separation of the tissues using suitable glass capillaries.At the beginning lupin was chosen because it had higher IAA-oxidase activity than pea, bean, oat or barley seedlings. At the time, it was thought that growth was mainly controlled through auxin catabolism (a fruitful line involving peroxidases was developed later). However, the etiolated hypocotyl was soon adopted preferentially by our group because of its qualities as a model for studying the relationship between hormone levels (auxin and ethylene) and growth. Our Portuguese colleagues have also used lupin as a model with successful results.⁹Bellow, we detail the landmarks of our research to date. Hypocotyl growth shows a characteristic pattern. Unlike plants grown in the light, in which all the cells along the hypocotyl elongate continuously throughout the growth period,^10,11 there is a steep growth gradient in the dark with an elongation zone just below the apex¹² (see Fig. 1 for details). This cell growth pattern in etiolated hypocotyls was described in lupin and then in Arabidopsis.¹¹ In this pattern, it is important to note that there is compensation along the organ between the cell diameter and the cell wall thickness. Once the cell growth pattern was known, we investigated its relation with the level of two phytohormones, auxin and ethylene, which might participate in the growth regulation. Special attention was paid to the distribution of endogenous IAA and its relation with growth. The results showed good correlation between the auxin levels and the cell size.^13,14 Auxin from the apex appears to be responsible for hypocotyl growth, since decapitation of seedlings strongly reduced growth, which was restored after the application of exogenous IAA to the cut surface.¹⁵ In light of the fact that growth depended on auxin from the apex, we investigated the nature of the auxin transport and demonstrated that this transport is polarized and sensitive to inhibition by specific inhibitors of polar auxin transport (PAT) such as 2,3,5-triiodobenzoic acid and 1-N-naphthylphtalamic acid (NPA).^16,17 Basipetal PAT mainly occurred in the stele,¹⁵ while cells in the epidermis and outer cortex are the limiting factor in auxin-induced shoot growth.^18–20 The finding that during PAT auxin can move laterally from transporting cells in the stele to the outer tissues of the elongation zone¹⁵ could explain the apparent conflict between the localization of PAT and the auxin target cells for elongation. In fact, epidermal cells acted as a sink for lateral auxin movement (LAM).¹⁷Open in a separate windowFigure 1Distribution of growth and cell size along the hypocotyl in etiolated lupin seedlings. At 3 d, hypocotyls were marked with ink, delimiting four 5-mm long zones including the apical, middle and basal zones. The hypocotyl growth ceased at day 12 and almost no growth was observed in the basal zone after day 3. From 3 to 6 d the growth was localized between the apical and basal zones, while most growth occurring from 6 to 12 d was localized in apical and middle zones. The cell size represents the cell length and cell diameter (the cell wall excluded) and corresponds to the second cell layer of cortex near the vascular cylinder. Similar results were obtained in cells from epidermis and pith. In each zone the cell length increased and the cell diameter showed little change during hypocotyl ageing. The final size at the end of the growth period varied along the hypocotyl, the cells becoming shorter and broader from the apical to the basal zones. In spite of the fact that cell diameter increased basipetally, no significant variation in hypocotyl diameter was found along the organ during the growth period. A morphometric study revealed that cell wall thickness in the apical cells was twice that in the basal cells at the end of the growth period i.e., the thinner apical cells had thicker cell walls, which may help explain the consistency of hypocotyl diameter along the organ.If PAT provides the auxin for growth and elongating growth is restricted to the apical region in etiolated hypocotyls, the question is: how does auxin accumulate in the elongation region?In a former study, we proposed that variations in auxin transport along actively growing lupin hypocotyl could produce such accumulation.²¹ Recently we extensively studied the variation of PAT along the lupin hypocotyls in seedlings of different ages, finding that certain parameters of PAT, such as transport intensity, polarity (basipetal vs acropetal) and sensitivity to NPA inhibition, showed a good correlation with the distribution of growth along the hypocotyl and its variation with ageing.²² These results suggest that a basipetally decreasing gradient in PAT along the hypocotyl may be responsible for the auxin distribution pattern controlling growth, since the existence of such a PAT gradient might generate the so-called barrier effect, which could produce an auxin gradient along the hypocotyl, the auxin content being higher in the apical elongation zone. To investigate whether these PAT variations can be explained in terms of auxin carrier distribution, we isolated three genes coding for auxin influx (LaAUX1) and efflux (LaPIN1 and LaPIN3) carriers, and studied their expression in different tissues along the hypocotyl at different ages.²³ The expression of LaAUX1 and LaPIN3 occurred both in the stele and in the outer tissues, while the expression of LaPIN1 was restricted to the stele and showed a basipetally decreasing gradient along the hypocotyl. The decisive role ascribed to PIN1 in polar auxin transport due to its localization in the basal end of transporting cells,²⁴ and the existence of such a gradient in the expression of LaPIN1 support the hypothesis of a barrier effect (generated by decreasing auxin transport) previously proposed as being responsible for the auxin gradient which controls the growth pattern in etiolated lupin hypocotyls.The acid-growth theory of auxin action was also tested, observing that the elongation growth of etiolated hypocotyl segments of lupin was stimulated by acid pH and IAA. Both factors stimulated growth in a more than additive way, suggesting a synergistic action between them.²⁵ The recent finding of a soluble auxin receptor (intracellular) reinforces the interest of the above study (which has remained a “sleeping beauty”) because pH affects IAA uptake.There are still several questions that must be answered before we can fully understand the growth pattern exhibited by etiolated lupin hypocotyls. Thus, as regards the cause of the PAT gradient, other factors besides the LaPIN1 gradient must be considered. For example, auxin carriers such as some phosphoglycoproteins (PGP), are also expressed differentially along the Arabidopsis hypocotyl and specific PIN-PGP pairings influence PAT by modulating the rates of cellular auxin movement.⁷ The pathway (symplast or apoplast) and mechanism of LAM remains unknown. Although alternative mechanisms have been proposed,²⁶ a previous study in lupin¹⁵ suggested that LAM is a diffusive process and that the IAA metabolism observed in the outer tissues might generate the radial gradient of auxin necessary for the maintenance of its lateral flow. It is thought that this metabolism of IAA occurs once the hormonal action is completed.^25,27 Although NPA does not inhibit LAM, the involvement of auxin efflux carriers cannot be discarded. In fact, the role of PIN carriers in lateral auxin transport towards and from the stele has been described in the root.²⁸ Other phytohormones besides auxin can modulate hypocotyl growth. Thus, the ethylene production rate, the 1-aminocyclopropane-1-carboxylic acid (ACC) content and the ACC oxidase activity decreased along the hypocotyl during the hypocotyl growth period.²⁹ Sensitivity to exogenous ethylene varied during growth, the young apical region being less sensitive than the older basal region.³⁰ Ethylene modified the cell growth pattern in the different tissues.³¹ The ethylene-induced lupin hypocotyl thickening was irreversible and mainly due to an increase in cell diameter. However, the inhibition of hypocotyl elongation produced by ethylene was reversible and involved irreversible inhibition of cell division and, paradoxically, stimulation of cell elongation to produce cells longer than those of the control.³²Studies in Arabidopsis showed that the hypocotyl growth in both light- and dark-grown plants is a process driven by cross-talk between multiple hormones. Interactions between auxins, ethylene, gibberellins and brassinosteroids have been described.^33,34 We think that the etiolated lupin hypocotyl remains a suitable model for confirming some of these results and for opening up new approaches in phytohormone research.     

Premarin improves memory, prevents scopolamine-induced amnesia and increases number of basal forebrain choline acetyltransferase positive cells in middle-aged surgically menopausal rats

Conjugated equine estrogen (CEE) is the most commonly prescribed estrogen therapy, and is the estrogen used in the Women's Health Initiative study. While in-vitro studies suggest that CEE is neuroprotective, no study has evaluated CEE's effects on a cognitive battery and brain immunohistochemistry in an animal model. The current experiment tested whether CEE impacted: I) spatial learning, reference memory, working memory and long-term retention, as well as ability to handle mnemonic delay and interference challenges; and, II) the cholinergic system, via pharmacological challenge during memory testing and ChAT-immunoreactive cell counts in the basal forebrain. Middle-aged ovariectomized (Ovx) rats received chronic cyclic injections of either Oil (vehicle), CEE-Low (10 μg), CEE-Medium (20 μg) or CEE-High (30 μg) treatment. Relative to the Oil group, all three CEE groups showed less overnight forgetting on the spatial reference memory task, and the CEE-High group had enhanced platform localization during the probe trial. All CEE groups exhibited enhanced learning on the spatial working memory task, and CEE dose-dependently protected against scopolamine-induced amnesia with every rat receiving the highest CEE dose maintaining zero errors after scopolamine challenge. CEE also increased number of ChAT-immunoreactive neurons in the vertical diagonal band of the basal forebrain. Neither the ability to remember after a delay nor interference, nor long-term retention, was influenced by the CEE regimen used in this study. These findings are similar to those reported previously for 17 β-estradiol, and suggest that CEE can provide cognitive benefits on spatial learning, reference and working memory, possibly through cholinergic mechanisms.     

Thermal biology of Phymaturus lizards: evolutionary constraints or lack of environmental variation?

Several aspects of the biology of Phymaturus lizards including their herbivorous diet, specialized microhabitat use, and viviparous reproductive mode are highly conserved within the group. Here, we explore two aspects of Phymaturus thermal biology and test for the co-evolution among aspects of the thermal biology in these lizards, such as thermal preferenda and critical temperatures. Secondly, we explore correlations among variation in thermal biology with elevation and latitude. To do so, we used phylogenetically based comparative analyses (PCM) together with conventional statistics. Our results show that thermal biology for Phymaturus is conservative and our data do not suggest the co-evolution of thermal variables. Moreover, we detected low levels of variation in the thermal parameters studied, and no clear relationships between climatic and thermal variables. As a significant association between climatic and thermal variables could be demonstrated for a set of syntopic Liolaemus lizards, we suggest that thermal biology in Phymaturus lizards may be evolutionarily or ecologically constrained.     

Encapsulation of an Agrobacterium radiobacter extract containing d-hydantoinase and d-carbamoylase activities into alginate–chitosan polyelectrolyte complexes: Preparation of the biocatalyst

Alginate–chitosan polyelectrolyte complexes (PECs) have been used for the first time as a suitable matrix for coimmobilisation of enzymes to reproduce a multistep enzymatic route for production of d-amino acids. Encapsulation of a crude cell extract from Agrobacterium radiobacter containing d-hydantoinase and d-carbamoylase activities into the PECs with negligible leakage from the formed capsules was accomplished. All results in this study indicate that the preparation of the biocatalyst (preparation method and chitosan characteristics) play a key role in the biocatalyst's properties. The most suitable biocatalysts were prepared using a chitosan with a medium molecular weight (600 kDa) and a degree of deacetylation of 0.9. For all of the preparation conditions under study, an encapsulation yield of around 60% was achieved and the enzymatic activity yields ranged from 30 to 80% for d-hydantoinase activity and from 40 to 128% for d-carbamoylase activity relative to the activities of the soluble extract. All of the biocatalysts were able to hydrolyze l,d-hydroxyphenylhydantoin into p-hydroxyphenylglycine with yields ranging from 30 to 80%.     

Characterization of the TRBP domain required for Dicer interaction and function in RNA interference

Background  

Dicer, Ago2 and TRBP are the minimum components of the human RNA-induced silencing complex (RISC). While Dicer and Ago2 are RNases, TRBP is the double-stranded RNA binding protein (dsRBP) that loads small interfering RNA into the RISC. TRBP binds directly to Dicer through its C-terminal domain.     

Effects of arsenic (As) exposure on the antioxidant status of gills of the zebrafish Danio rerio (Cyprinidae)

In fishes, arsenic (As) is absorbed via the gills and is capable of causing disturbance to the antioxidant system. The objective of present study was to evaluate antioxidant responses after As exposure in gills of zebrafish (Danio rerio, Cyprinidae). Fish were exposed for 48 h to three concentration of As, including the highest As concentration allowed by current Brazilian legislation (10 μg As/L). A control group was exposed to tap water (pH 8.0; 26 °C; 7.20 mg O₂/L). As exposure resulted in (1) an increase (p < 0.05) of glutathione (GSH) levels after exposure to 10 and 100 μg As/L, (2) an increase of the glutamate cysteine ligase (GCL) activity in the same concentrations (p < 0.05), (3) no significant differences in terms of glutathione reductase, glutathione-S-transferase and catalase activities; (4) a significantly lower (p < 0.05) oxygen consumption after exposure to 100 μg As/L; (4) no differences in terms of oxygen reactive species generation and lipid peroxidation content (p > 0,05). In the gills, only inorganic As was detected. Overall, it can be concluded that As affected the antioxidant responses increasing GCL activity and GSH levels, even at concentration considered safe by Brazilian legislation.     

A Prospective Nested Case-Control Study of Dengue in Infants: Rethinking and Refining the Antibody-Dependent Enhancement Dengue Hemorrhagic Fever Model

Background

Dengue hemorrhagic fever (DHF) is the severe and life-threatening syndrome that can develop after infection with any one of the four dengue virus (DENV) serotypes. DHF occurs almost exclusively in individuals with secondary heterologous DENV infections and infants with primary DENV infections born to dengue immune mothers. The widely accepted explanation for the pathogenesis of DHF in these settings, particularly during infancy, is antibody-dependent enhancement (ADE) of DENV infection.

Methods and Findings

We conducted a prospective nested case-control study of DENV infections during infancy. Clinical data and blood samples were collected from 4,441 mothers and infants in up to two pre-illness study visits, and surveillance was performed for symptomatic and inapparent DENV infections. Pre-illness plasma samples were used to measure the associations between maternally derived anti-DENV3 antibody-neutralizing and -enhancing capacities at the time of DENV3 infection and development of infant DHF.The study captured 60 infants with DENV infections across a wide spectrum of disease severity. DENV3 was the predominant serotype among the infants with symptomatic (35/40) and inapparent (15/20) DENV infections, and 59/60 infants had a primary DENV infection. The estimated in vitro anti-DENV3 neutralizing capacity at birth positively correlated with the age of symptomatic primary DENV3 illness in infants. At the time of symptomatic DENV3 infection, essentially all infants had low anti-DENV3 neutralizing activity (50% plaque reduction neutralizing titers [PRNT₅₀] ≤50) and measurable DENV3 ADE activity. The infants who developed DHF did not have significantly higher frequencies or levels of DENV3 ADE activity compared to symptomatic infants without DHF. A higher weight-for-age in the first 3 mo of life and at illness presentation was associated with a greater risk for DHF from a primary DENV infection during infancy.

Conclusions

This prospective nested case-control study of primarily DENV3 infections during infancy has shown that infants exhibit a full range of disease severity after primary DENV infections. The results support an initial in vivo protective role for maternally derived antibody, and suggest that a DENV3 PRNT₅₀ >50 is associated with protection from symptomatic DENV3 illness. We did not find a significant association between DENV3 ADE activity at illness onset and the development of DHF compared with less severe symptomatic illness. The results of this study should encourage rethinking or refinement of the current ADE pathogenesis model for infant DHF and stimulate new directions of research into mechanisms responsible for the development of DHF during infancy.

Trial registration

ClinicalTrials.gov {"type":"clinical-trial","attrs":{"text":"NCT00377754","term_id":"NCT00377754"}}NCT00377754 Please see later in the article for the Editors'' Summary     

The cellular prion protein and its role in Alzheimer disease

The cellular prion protein (PrP^C) is a membrane-bound glycoprotein especially abundant in the central nervous system (CNS). The scrapie prion protein (PrP^Sc, also termed prions) is responsible of transmissible spongiform encephalopathies (TSE), a group of neurodegenerative diseases which affect humans and other mammal species, although the presence of PrP^C is needed for the establishment and further evolution of prions.The present work compares the expression and localization of PrP^C between healthy human brains and those suffering from Alzheimer disease (AD).In both situations we have observed a rostrocaudal decrease in the amount of PrP^C within the CNS, both by immunoblotting and immunohistochemistry techniques. PrP^C is higher expressed in our control brains than in AD cases. There was a neuronal loss and astogliosis in our AD cases. There was a tendency of a lesser expression of PrP^C in AD cases than in healthy ones. And in AD cases, the intensity of the expression of the unglycosylated band is higher than the di- and monoglycosylated bands.With regards to amyloid plaques, those present in AD cases were positively labeled for PrP^C, a result which is further supported by the presence of PrP^C in the amyloid plaques of a transgenic line of mice mimicking AD.The work was done according to Helsinki Declaration of 1975, and approved by the Ethics Committee of the Faculty of Medicine of the University of Navarre.Key words: cellular prion protein, Alzheimer disease, transgenic mice     

Anemia of Inflammation Is Related to Cognitive Impairment among Children in Leyte,The Philippines

Background

Many studies have addressed the relationship between iron deficiency anemia (IDA) and cognitive impairment, but none have evaluated the role of non-iron deficiency anemia (NIDA). One of the main causes of NIDA in developing countries is AI, largely due to infectious diseases, whereby iron is shunted away from bio-available forms to storage forms, making it less accessible for use by host tissues. The objective of this study was to determine the effect of NIDA, due largely to AI in this context, on cognitive function after adjustment for potential confounders.

Methodology

This cross-sectional study was conducted in Leyte, The Philippines among 322 children ages 7–18 years. Blood samples were collected and analyzed at the time of cognition testing. Three stool samples were collected and evaluated by the Kato Katz method for quantitative assessment for Schistosoma japonicum and geo-helminth infection. Socio-economic status (SES) was evaluated by survey. Linear regression models were used to quantify the adjusted relationship between performance in different cognitive domains and both IDA and NIDA.

Principal Findings

After adjusting for age, sex, SES and nutritional status, children in the NIDA had lower scores on the PNIT (P = <0.05) and the WRAML memory domain (P<0.05) compared to children in the non-anemic group. Children in the IDA had lower performance on the PNIT compared to the non-anemic group after controlling for potential confounders (P<0.05).

Conclusions

NIDA, predominantly due to AI in this context, was related to lower performance on two tests of cognitive function. This is likely due to decreased delivery of iron to host tissues in this context, including the CNS.