Your search keyword '"Life Cycle Stages physiology"' showing total 1,390 results

201. Distinct 3' UTRs regulate the life-cycle-specific expression of two TCTP paralogs in Trypanosoma brucei .

Author

Jojic B, Amodeo S, Bregy I, and Ochsenreiter T

Subjects

3' Untranslated Regions, Biomarkers, Tumor genetics, Life Cycle Stages physiology, Protozoan Proteins genetics, RNA, Messenger genetics, RNA, Messenger metabolism, Tumor Protein, Translationally-Controlled 1, Biomarkers, Tumor biosynthesis, Protozoan Proteins biosynthesis, Trypanosoma brucei brucei genetics, Trypanosoma brucei brucei metabolism

Abstract

The translationally controlled tumor protein (TCTP; also known as TPT1 in mammals) is highly conserved and ubiquitously expressed in eukaryotes. It is involved in growth and development, cell cycle progression, protection against cellular stresses and apoptosis, indicating the multifunctional role of the protein. Here, for the first time, we characterize the expression and function of TCTP in the human and animal pathogen, Trypanosoma brucei We identified two paralogs ( TCTP1 and TCTP2 ) that are differentially expressed in the life cycle of the parasite. The genes have identical 5' untranslated regions (UTRs) and almost identical open-reading frames. The 3'UTRs differ substantially in sequence and length, and are sufficient for the exclusive expression of TCTP1 in procyclic- and TCTP2 in bloodstream-form parasites. Furthermore, we characterize which parts of the 3'UTR are needed for TCTP2 mRNA stability. RNAi experiments demonstrate that TCTP1 and TCTP2 expression is essential for normal cell growth in procyclic- and bloodstream-form parasites, respectively. Depletion of TCTP1 in the procyclic form cells leads to aberrant cell and mitochondrial organelle morphology, as well as enlarged, and a reduced number of, acidocalcisomes., Competing Interests: Competing interestsThe authors declare no competing or financial interests., (© 2018. Published by The Company of Biologists Ltd.)

Published

2018

202. The AmP project: Comparing species on the basis of dynamic energy budget parameters.

Author

Marques GM, Augustine S, Lika K, Pecquerie L, Domingos T, and Kooijman SALM

Subjects

Animals, Biological Evolution, Computational Biology, Crustacea physiology, Databases, Factual, Fishes physiology, Life Cycle Stages physiology, Species Specificity, Biodiversity, Energy Metabolism, Models, Biological

Abstract

We developed new methods for parameter estimation-in-context and, with the help of 125 authors, built the AmP (Add-my-Pet) database of Dynamic Energy Budget (DEB) models, parameters and referenced underlying data for animals, where each species constitutes one database entry. The combination of DEB parameters covers all aspects of energetics throughout the full organism's life cycle, from the start of embryo development to death by aging. The species-specific parameter values capture biodiversity and can now, for the first time, be compared between animals species. An important insight brought by the AmP project is the classification of animal energetics according to a family of related DEB models that is structured on the basis of the mode of metabolic acceleration, which links up with the development of larval stages. We discuss the evolution of metabolism in this context, among animals in general, and ray-finned fish, mollusks and crustaceans in particular. New DEBtool code for estimating DEB parameters from data has been written. AmPtool code for analyzing patterns in parameter values has also been created. A new web-interface supports multiple ways to visualize data, parameters, and implied properties from the entire collection as well as on an entry by entry basis. The DEB models proved to fit data well, the median relative error is only 0.07, for the 1035 animal species at 2018/03/12, including some extinct ones, from all large phyla and all chordate orders, spanning a range of body masses of 16 orders of magnitude. This study is a first step to include evolutionary aspects into parameter estimation, allowing to infer properties of species for which very little is known., Competing Interests: The authors have declared that no competing interests exist.

Published

2018

203. Infection of Anopheles aquasalis from symptomatic and asymptomatic Plasmodium vivax infections in Manaus, western Brazilian Amazon.

Author

Martins-Campos KM, Kuehn A, Almeida A, Duarte APM, Sampaio VS, Rodriguez ÍC, da Silva SGM, Ríos-Velásquez CM, Lima JBP, Pimenta PFP, Bassat Q, Müller I, Lacerda M, Monteiro WM, and Barbosa Guerra MDGV

Subjects

Adult, Animals, Anopheles genetics, Anopheles physiology, Brazil epidemiology, Cross-Sectional Studies, Disease Eradication, Endemic Diseases, Female, Humans, Life Cycle Stages physiology, Malaria, Vivax blood, Malaria, Vivax parasitology, Malaria, Vivax transmission, Male, Middle Aged, Mosquito Vectors parasitology, Oocysts physiology, Plasmodium vivax genetics, Prevalence, Real-Time Polymerase Chain Reaction, Anopheles parasitology, Asymptomatic Infections epidemiology, Malaria, Vivax epidemiology, Plasmodium vivax physiology

Abstract

Background: Asymptomatic individuals are one of the major challenges for malaria elimination programs in endemic areas. In the absence of clinical symptoms and with a lower parasite density they constitute silent reservoirs considered important for maintaining transmission of human malaria. Studies from Brazil have shown that infected individuals may carry these parasites for long periods., Results: Patients were selected from three periurban endemic areas of the city of Manaus, in the western Brazilian Amazon. Symptomatic and asymptomatic patients with positive thick blood smear and quantitative real-time PCR (qPCR) positive for Plasmodium vivax were invited to participate in the study. A standardised pvs25 gene amplification by qPCR was used for P. vivax gametocytes detection. Anopheles aquasalis were fed using membrane feeding assays (MFA) containing blood from malaria patients. Parasitemia of 42 symptomatic and 25 asymptomatic individuals was determined by microscopic examination of blood smears and qPCR. Parasitemia density and gametocyte density were assessed as determinants of infection rates and oocysts densities. A strong correlation between gametocyte densities (microscopy and molecular techniques) and mosquito infectivity (P < 0.001) and oocysts median numbers (P < 0.05) was found in both groups. The ability to infect mosquitoes was higher in the symptomatic group (41%), but infectivity in the asymptomatic group was also seen (1.42%)., Conclusions: Although their infectivity to mosquitoes is relatively low, given the high prevalence of P. vivax asymptomatic carriers they are likely to play and important role in malaria transmission in the city of Manaus. The role of asymptomatic infections therefore needs to be considered in future malaria elimination programs in Brazil.

Published

2018

204. Comparative survival of the engorged stages of Amblyomma cajennense sensu stricto and Amblyomma sculptum under different laboratory conditions.

Author

Labruna MB

Subjects

Animals, Brazil, Ecosystem, Female, Humidity, Molting physiology, Nymph physiology, Oviposition physiology, Seasons, South America, Ixodidae physiology, Larva physiology, Life Cycle Stages physiology

Abstract

Recent studies indicated that the taxon Amblyomma cajennense (Fabricius, 1787) is a complex of 6 valid species, of which only two, Amblyomma cajennense sensu stricto (s.s.) and Amblyomma sculptum Berlese, 1888 are present in Brazil; the former species is found exclusively in areas of the Amazon biome, and A. sculptum mostly in the Cerrado biome. Populations of A. cajennense s.s. and A. sculptum are usually sustained by the same host species, and are found in many areas with similar temperature and photoperiod regimens. On the other hand, differences in the rainfall regimen and vegetation cover of the Amazon and Cerrado biomes, reflecting different vapor saturation deficit of atmosphere in the soil, could be primary factors driving the geographical distribution of the two species. In this study, all developmental stages in the life cycle of A. cajennense s.s. and A. sculptum were exposed to different temperature, photoperiod, and relative humidity (65, 78 or 100%) regimens that simulated mean conditions during summer or winter of one area of the Amazon and one area of the Cerrado in Brazil. Ticks were also exposed to water immersion during different periods of time (24, 48, or 72 h). Our experiments showed that A. sculptum showed significantly higher molting success for engorged larvae and oviposition success for engorged females than A. cajennense s.s. when these engorged ticks were incubated at higher saturation deficit conditions (65 and/or 78% RH with summer and winter mean temperatures). On the other hand, when ticks were immersed in water for 24, 48 or 72 h, there was a clear tendency for engorged stages (larvae, nymphs or females) of A. cajennense s.s. to have greater molting or oviposition success than A. sculptum. These results indicate that engorged stages of A. sculptum showed a greater capacity to survive under higher saturation deficit conditions (lower RH values associated with mean summer and winter temperatures), and engorged stages of A. cajennense s.s. had a greater capacity to survive under the highest moisture conditions, namely immersed in water for a relatively short period (24-72 h). When applied to the natural distributions of A. cajennense s.s. and A. sculptum in Brazil, we can infer that the former species is more adapted to the humid conditions of the Amazon biome, where the soil inside forests is quite moist throughout the year, and often swampy or flooded during the raining season. On the other hand, immature stages of A. sculptum are more adapted to the drought period of the Cerrado biome, when higher saturation deficit conditions prevail on the soil., (Copyright © 2018 Elsevier GmbH. All rights reserved.)

Published

2018

205. Anatomical and phenological implications of the relationship between Schinus polygama (Cav.) (Cabrera) and the galling insect Calophya rubra (Blanchard).

Author

Guedes LM, Aguilera N, Ferreira BG, Becerra J, Hernández V, and Isaias RMS

Subjects

Anacardiaceae anatomy & histology, Animals, Chile, Life Cycle Stages physiology, Plant Stems anatomy & histology, Plant Stems parasitology, Anacardiaceae parasitology, Hemiptera physiology, Plant Tumors parasitology

Abstract

The success of galling insects could be determined by synchronisation with host plant phenology and climate conditions, ensuring suitable oviposition sites for gall induction and food resources for their survival. The anatomical, histochemical and phenological synchronisation strategies between Calophya rubra (Blanchard) (Hemiptera: Psylloidea) and its host, the evergreen plant Schinus polygama (Cav.) (Cabrera) (Anacardiaceae), in the Mediterranean climate of southern Chile was evaluated and compared to that of the congeneric C. cf. duvauae (Scott) from Brazil and closely related host plant S. engleri in a subtropical climate. Anatomical, histometric, histochemical and vegetative phenology studies of the stem and galls were conducted from June 2015 to December 2016. Based on the anatomical, histometric and histochemical analysis, the conical stem gall traits imply gains over the non-galled stem toward the galling insect survival, but the maintenance of phellem, secretory ducts and pith indicate conservative developmental traits that cannot be manipulated by C. rubra. Our results indicate that the conditions of the Mediterranean climate zone limit C. rubra immature activity during unfavourable periods, probably determining a diapause period and a univoltine life cycle, which are peculiarities of the S. polygama- C. rubra system. The synchronisation between development and seasonality confers peculiarities to the S. polygama- C. rubra system in the Mediterranean climate zone., (© 2018 German Society for Plant Sciences and The Royal Botanical Society of the Netherlands.)

Published

2018

206. The phylogenetic position of Choerodonicola Cribb, 2005 (Digenea: Opecoelidae) with a partial life-cycle for a new species from the blue-barred parrotfish Scarus ghobban Forsskål (Scaridae) in Moreton Bay, Australia.

Author

Martin SB, Cribb TH, Cutmore SC, and Huston DC

Subjects

Animals, Bays, DNA, Ribosomal genetics, DNA, Ribosomal Spacer genetics, Queensland, Species Specificity, Trematoda anatomy & histology, Trematoda genetics, Trematoda growth & development, Life Cycle Stages physiology, Perciformes parasitology, Phylogeny, Trematoda classification

Abstract

Choerodonicola Cribb, 2005 is a minor genus of opecoelid trematodes defined for species with exceptionally small eggs but otherwise generalised morphology. Four species are currently recognised, all from fishes collected in Japanese waters but each from different perciform families: a labrid, a scarid, a sparid and pinguipeds. We report on a new species, Choerodonicola arothokoros n. sp., from the blue-barred parrotfish Scarus ghobban Forsskål (Scaridae) collected in subtropical waters of Moreton Bay, south-east Queensland, Australia. Using genetic sequence data for the ITS2 rDNA marker, we matched adult C. arothokoros to intramollsucan stages discovered in an intertidal gastropod Herpetopoma atratum (Gmelin) (Vetigastropoda: Chilodontidae) collected in close proximity to the fish hosts. Notably, the cercariae lack a penetration stylet and are among the smallest known in the Opecoelidae. We provide the first assessment of the phylogenetic position of Choerodonicola based on sequence data generated for the phylogenetically informative 18S and 28S rRNA coding regions, for C. arothokoros and also C. renko Machida, 2014, which we recollected from the yellowback seabream Dentex hypselosomus Bleeker from the fish market in Minabe, Wakayama Prefecture, Japan. In our analyses, species of Choerodonicola resolved to neither of the major marine Plagioporinae (sensu lato) clades, clustering instead with Trilobovarium parvvatis Martin, Cutmore & Cribb, 2017, Podocotyloides parupenei (Manter, 1963) Pritchard, 1966 and Macvicaria magellanica Laskowski, Jeżewski & Zdzitowiecki, 2013. This clade is phylogenetically distinctive such that it has the potential to be recognised as a new opecoelid subfamily, but further investigation is required to establish the bounds for such a grouping and to determine the morphological and/or life-history patterns reflected by the phylogeny. Finally, we propose C. interruptus (Manter 1954) n. comb. for a species previously recognised in Plagioporus Stafford, 1904 and known only from Pseudolabrus miles (Schneider & Forster), a labrid endemic to New Zealand.

Published

2018

207. Multi-tissue GAL4-mediated gene expression in all Anopheles gambiae life stages using an endogenous polyubiquitin promoter.

Author

Adolfi A, Pondeville E, Lynd A, Bourgouin C, and Lycett GJ

Subjects

Animals, Organ Specificity physiology, Anopheles genetics, Anopheles growth & development, Gene Expression Regulation physiology, Insect Proteins genetics, Insect Proteins metabolism, Life Cycle Stages physiology, Polyubiquitin genetics, Polyubiquitin metabolism, Promoter Regions, Genetic physiology, Transcription Factors genetics, Transcription Factors metabolism

Abstract

The ability to manipulate the Anopheles gambiae genome and alter gene expression effectively and reproducibly is a prerequisite for functional genetic analysis and for the development of novel control strategies in this important disease vector. However, in vivo transgenic analysis in mosquitoes is limited by the lack of promoters active ubiquitously. To address this, we used the GAL4/UAS system to investigate the promoter of the An. gambiae Polyubiquitin-c (PUBc) gene and demonstrated its ability to drive expression in mosquito cell culture before incorporation into An. gambiae transgenic driver lines. To generate such lines, piggyBac-mediated insertion was used to identify genomic regions able to sustain widespread expression and to create φC31 docking lines at these permissive sites. Patterns of expression induced by PUBc-GAL4 drivers carrying single intergenic insertions were assessed by crossing with a novel responder UAS-mCD8:mCherry line that was created by φC31-mediated integration. Amongst the drivers created at single, unique chromosomal integration loci, two were isolated that induced differential expression levels in a similar multiple-tissue spatial pattern throughout the mosquito life cycle. This work expands the tools available for An. gambiae functional analysis by providing a novel promoter for investigating phenotypes resulting from widespread multi-tissue expression, as well as identifying and tagging genomic sites that sustain broad transcriptional activity., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2018

208. Inositol polyphosphate multikinase regulation of Trypanosoma brucei life stage development.

Author

Cestari I, Anupama A, and Stuart K

Subjects

Animals, Energy Metabolism, Inositol Phosphates metabolism, Life Cycle Stages physiology, Parasites metabolism, Phosphorylation, Signal Transduction, Trypanosoma brucei brucei genetics, Trypanosoma brucei brucei growth & development, Phosphotransferases (Alcohol Group Acceptor) metabolism, Phosphotransferases (Alcohol Group Acceptor) physiology, Trypanosoma brucei brucei metabolism

Abstract

Many cellular processes change during the Trypanosoma brucei life cycle as this parasite alternates between the mammalian host and tsetse fly vector. We show that the inositol phosphate pathway helps regulate these developmental changes. Knockdown of inositol polyphosphate multikinase (IPMK), which phosphorylates Ins(1,4,5)P3 and Ins(1,3,4,5)P4, resulted in changes in bloodstream forms that are characteristic of insect stage procyclic forms. These changes include expression of the procyclic surface coat, up-regulation of RNA-binding proteins that we show to regulate stage-specific transcripts, and activation of oxidative phosphorylation with increased ATP production in bloodstream forms. These changes were accompanied by development of procyclic morphology, which also occurred by the expression of a catalytically inactive IPMK, implying that regulation of these processes entails IPMK activity. Proteins involved in signaling, protein synthesis and turnover, and metabolism were affinity-enriched with the IPMK substrate or product. Developmental changes associated with IPMK knockdown or catalytic inactivation reflected processes that are enriched with inositol phosphates, and chemical and genetic perturbation of these processes affected T. brucei development. Hence, IPMK helps regulate T. brucei development, perhaps by affecting inositol phosphate interactions with proteins of the regulatory network that controls energy metabolism and development.

Published

2018

209. Thermal strategies vary with life history stage.

Author

Truebano M, Fenner P, Tills O, Rundle SD, and Rezende EL

Subjects

Animals, Gastropoda growth & development, Heat-Shock Response, Larva physiology, Life Cycle Stages physiology, Gastropoda physiology, Hot Temperature

Abstract

With both global surface temperatures and the incidence and intensity of extreme temperature events projected to increase, the assessment of species' sensitivity to chronic and acute changes in temperature has become crucial. Sensitivity predictions are based predominantly on adult responses, despite the fact that early life stages may be more vulnerable to thermal challenge. Here, we compared the sensitivity of different life history stages of the intertidal gastropod Littorina obtusata using thermal death time curves, which incorporate the intensity and duration of heat stress, and used these to calculate upper critical thermal limits (CT max ) and sensitivity to temperature change ( z ). Early (larval) life stages had both a lower CT max and a lower z than adults, suggesting they are less good at withstanding short-term extreme thermal challenges but better able to survive moderate temperatures in the long term. This result supports the predicted trade-off between acute and chronic tolerance to thermal stress, and is consistent with the different thermal challenges that these stages encounter in the intertidal zone. We conclude that different life history stages employ different thermal strategies that may be adaptive. Our findings caution against the use of predictions of the impact of global warming that are based on only adult responses and, hence, which may underestimate vulnerability., Competing Interests: Competing interestsThe authors declare no competing or financial interests., (© 2018. Published by The Company of Biologists Ltd.)

Published

2018

210. Blood flukes Cardicola parvus and C. laruei (Trematoda: Aporocotylidae): life cycles and cryptic infection in spotted seatrout, Cynoscion nebulosus (Teleost: Sciaenidae).

Author

Siegel SV, Rivero AV, Oberstaller J, Colon BL, de Buron I, and Kyle DE

Subjects

Animals, Atlantic Ocean, Cercaria isolation & purification, Genotype, Life Cycle Stages physiology, Oocysts isolation & purification, Perciformes parasitology, Trematoda genetics, Polychaeta parasitology, Trematoda physiology, Trematode Infections parasitology, Trout parasitology

Abstract

Aporocotylidae comprises a diverse family of fish blood flukes, with adults found in blood or body cavity of marine, brackish, or freshwater fish. Aporocotylids are unique among the Digenea with many developing in polychaetes. The life cycle has been elucidated for only a few species that develop in polychaetes from marine/brackish environments and none for western Atlantic aporocotylids. The basis for this study was observations of blood fluke larvae in annelids from South Carolina, USA in 1982 prior to possible usage of molecular tools to specifically identify parasite larvae. Recent description of aporocotylid species and genotyping tools prompted revisiting original collection sites to examine polychaetes and fish as potential hosts. Polycirrid Enoplobranchus sanguineus and terebellids Amphitrite ornata, and Terebella lapidaria revealed infections with aporocotylid larvae. Adult blood flukes were also collected from fish commonly encountered in the same habitat: spotted seatrout (Cynoscion nebulosus), red drum (Sciaenops ocellatus), black drum (Pogonias cromis), and Atlantic croaker (Micropogonias undulatus). Sporocysts containing cercariae were found in individuals of each annelid species. Adult Cardicola parvus were found in spotted seatrout and Atlantic croaker, C. laruei in spotted seatrout, C. currani in red drum, and C. palmeri in black drum. Genotype analysis of ITS-2 and lsrDNA of all forms confirmed conspecific infections by C. parvus in E. sanguineus and A. ornata and C. laruei in T. lapidaria. This is the first description of complete life cycles of aporocotylids in the Western Atlantic and first evidence of cryptic infections of Cy. nebulosus with C. parvus., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2018

211. Involvement of STI1 protein in the differentiation process of Trypanosoma cruzi.

Author

Schmidt JC, Manhães L, Fragoso SP, Pavoni DP, and Krieger MA

Subjects

Fluorescent Antibody Technique, Indirect, Gene Knockout Techniques, Gene Silencing, Heat-Shock Proteins genetics, Life Cycle Stages genetics, Life Cycle Stages physiology, Mutation, Protozoan Proteins metabolism, Stress, Physiological, Trypanosoma cruzi chemistry, Trypanosoma cruzi ultrastructure, Heat-Shock Proteins metabolism, Protozoan Proteins genetics, Trypanosoma cruzi growth & development, Trypanosoma cruzi physiology

Abstract

The protozoan Trypanosoma cruzi is a parasite exposed to several environmental stressors inside its invertebrate and vertebrate hosts. Although stress conditions are involved in its differentiation processes, little information is available about the stress response proteins engaged in these activities. This work reports the first known association of the stress-inducible protein 1 (STI1) with the cellular differentiation process in a unicellular eukaryote. Albeit STI1 expression is constitutive in epimastigotes and metacyclic trypomastigotes, higher protein levels were observed in late growth phase epimastigotes subjected to nutritional stress. Analysis by indirect immunofluorescence revealed that T. cruzi STI1 (TcSTI1) is located throughout the cell cytoplasm, with some cytoplasmic granules appearing in greater numbers in late growing epimastigotes and late growing epimastigotes subjected to nutritional stress. We observed that part of the fluorescence signal from both TcSTI1 and TcHSP70 colocalized around the nucleus. Gene silencing of sti1 in Trypanosoma brucei did not affect cell growth. Similarly, the growth of T. cruzi mutant parasites with a single allele sti1 gene knockout was not affected. However, the differentiation of epimastigotes in metacyclic trypomastigotes (metacyclogenesis) was compromised. Lower production rates and numbers of metacyclic trypomastigotes were obtained from the mutant parasites compared with the wild-type parasites. These data indicate that reduced levels of TcSTI1 decrease the rate of in vitro metacyclogenesis, suggesting that this protein may participate in the differentiation process of T. cruzi., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2018

212. Global change scenarios trigger carry-over effects across life stages and generations of the intertidal limpet, Siphonaria australis.

Author

Kessel GM and Phillips NE

Subjects

Animals, Embryo, Nonmammalian, Embryonic Development physiology, Larva, New Zealand, Seawater, Gastropoda embryology, Gastropoda growth & development, Gastropoda physiology, Global Warming, Life Cycle Stages physiology, Reproduction physiology, Temperature

Abstract

For organisms with complex life histories, carry-over effects (COEs) can manifest between life stages, when conditions experienced by one stage influence the next, as well as trans-generationally, when the parental environment affects offspring. Here we used multiple global change-associated stressors to examine both forms of COE simultaneously in an intertidal limpet with mixed development (i.e. planktonic larvae hatch from benthic egg masses). Adult Siphonaria australis were subjected to four treatments over four weeks: an ambient control, a treatment featuring elevated water temperature (25°C) and UVB (1.7 W m-2), a copper pollution treatment (5.0 μg L-1), and a treatment incorporating all three stressors. Egg masses laid by these adults were then redistributed among the same four treatments (producing 16 adult-to-egg treatment histories) and stressed until hatching. Finally, hatching larvae were reared under ambient conditions for 24 days. While adult survivorship was unaffected by treatment, embryonic viability in egg masses responded strongly to egg mass treatment, as well as parental stress exposure, therefore displaying trans-generational COEs. These trans-generational COEs interacted with COEs originating in egg masses to produce highly context-dependent hatching sizes and larval growth. This demonstrates that the performance of a given organism at a given time reflects not only conditions experienced during embryonic development, but also those of the parental generation, and suggests that COEs play an important but underestimated role in responses to global change scenarios.

Published

2018

213. Comparative Heterochromatin Profiling Reveals Conserved and Unique Epigenome Signatures Linked to Adaptation and Development of Malaria Parasites.

Author

Fraschka SA, Filarsky M, Hoo R, Niederwieser I, Yam XY, Brancucci NMB, Mohring F, Mushunje AT, Huang X, Christensen PR, Nosten F, Bozdech Z, Russell B, Moon RW, Marti M, Preiser PR, Bártfai R, and Voss TS

Subjects

Adaptation, Physiological genetics, Adaptation, Physiological physiology, Animals, Antigenic Variation genetics, Antigens, Protozoan genetics, Cell Proliferation, Chromobox Protein Homolog 5, Disease Models, Animal, Female, Gene Expression Regulation, Gene Silencing, Host-Parasite Interactions genetics, Host-Parasite Interactions physiology, Humans, Life Cycle Stages genetics, Life Cycle Stages physiology, Malaria, Falciparum parasitology, Mice, Mice, Inbred BALB C, Parasites genetics, Phylogeny, Plasmodium classification, Plasmodium falciparum genetics, Plasmodium falciparum metabolism, Protozoan Proteins genetics, Protozoan Proteins metabolism, Sex Differentiation, Chromosomal Proteins, Non-Histone genetics, Chromosomal Proteins, Non-Histone metabolism, Epigenesis, Genetic genetics, Epigenomics, Gene Expression Profiling, Heterochromatin genetics, Plasmodium genetics, Plasmodium physiology

Abstract

Heterochromatin-dependent gene silencing is central to the adaptation and survival of Plasmodium falciparum malaria parasites, allowing clonally variant gene expression during blood infection in humans. By assessing genome-wide heterochromatin protein 1 (HP1) occupancy, we present a comprehensive analysis of heterochromatin landscapes across different Plasmodium species, strains, and life cycle stages. Common targets of epigenetic silencing include fast-evolving multi-gene families encoding surface antigens and a small set of conserved HP1-associated genes with regulatory potential. Many P. falciparum heterochromatic genes are marked in a strain-specific manner, increasing the parasite's adaptive capacity. Whereas heterochromatin is strictly maintained during mitotic proliferation of asexual blood stage parasites, substantial heterochromatin reorganization occurs in differentiating gametocytes and appears crucial for the activation of key gametocyte-specific genes and adaptation of erythrocyte remodeling machinery. Collectively, these findings provide a catalog of heterochromatic genes and reveal conserved and specialized features of epigenetic control across the genus Plasmodium., (Copyright © 2018 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2018

214. Life Cycle, Ultrastructure, and Phylogeny of New Diplonemids and Their Endosymbiotic Bacteria.

Author

Tashyreva D, Prokopchuk G, Votýpka J, Yabuki A, Horák A, and Lukeš J

Subjects

Bacteria genetics, Life Cycle Stages physiology, Phylogeny, RNA, Ribosomal, 18S genetics, Meiotic Prophase I physiology, Symbiosis physiology

Abstract

Diplonemids represent a hyperdiverse and abundant yet poorly studied group of marine protists. Here we describe two new members of the genus Diplonema (Diplonemea, Euglenozoa), Diplonema japonicum sp. nov. and Diplonema aggregatum sp. nov., based on life cycle, morphology, and 18S rRNA gene sequences. Along with euglenozoan apomorphies, they contain several unique features. Their life cycle is complex, consisting of a trophic stage that is, following the depletion of nutrients, transformed into a sessile stage and subsequently into a swimming stage. The latter two stages are characterized by the presence of tubular extrusomes and the emergence of a paraflagellar rod, the supportive structure of the flagellum, which is prominently lacking in the trophic stage. These two stages also differ dramatically in motility and flagellar size. Both diplonemid species host endosymbiotic bacteria that are closely related to each other and constitute a novel branch within Holosporales , for which a new genus, " Candidatus Cytomitobacter" gen. nov., has been established. Remarkably, the number of endosymbionts in the cytoplasm varies significantly, as does their localization within the cell, where they seem to penetrate the mitochondrion, a rare occurrence. IMPORTANCE We describe the morphology, behavior, and life cycle of two new Diplonema species that established a relationship with two Holospora -like bacteria in the first report of an endosymbiosis in diplonemids. Both endosymbionts reside in the cytoplasm and the mitochondrion, which establishes an extremely rare case. Within their life cycle, the diplonemids undergo transformation from a trophic to a sessile and eventually a highly motile swimming stage. These stages differ in several features, such as the presence or absence of tubular extrusomes and a paraflagellar rod, along with the length of the flagella. These morphological and behavioral interstage differences possibly reflect distinct functions in dispersion and invasion of the host and/or prey and may provide novel insight into the virtually unknown function of diplonemids in the oceanic ecosystem., (Copyright © 2018 Tashyreva et al.)

Published

2018

215. Gut Microbial Changes, Interactions, and Their Implications on Human Lifecycle: An Ageing Perspective.

Author

Vemuri R, Gundamaraju R, Shastri MD, Shukla SD, Kalpurath K, Ball M, Tristram S, Shankar EM, Ahuja K, and Eri R

Subjects

Aging drug effects, Animals, Anti-Bacterial Agents pharmacology, Anti-Bacterial Agents therapeutic use, Gastrointestinal Microbiome drug effects, Gastrointestinal Tract drug effects, Gastrointestinal Tract immunology, Gastrointestinal Tract microbiology, Humans, Immune System immunology, Life Cycle Stages drug effects, Prebiotics, Probiotics pharmacology, Probiotics therapeutic use, Aging immunology, Aging physiology, Gastrointestinal Microbiome immunology, Gastrointestinal Microbiome physiology, Life Cycle Stages immunology, Life Cycle Stages physiology

Abstract

Gut microbiota is established during birth and evolves with age, mostly maintaining the commensal relationship with the host. A growing body of clinical evidence suggests an intricate relationship between the gut microbiota and the immune system. With ageing, the gut microbiota develops significant imbalances in the major phyla such as the anaerobic Firmicutes and Bacteroidetes as well as a diverse range of facultative organisms, resulting in impaired immune responses. Antimicrobial therapy is commonly used for the treatment of infections; however, this may also result in the loss of normal gut flora. Advanced age, antibiotic use, underlying diseases, infections, hormonal differences, circadian rhythm, and malnutrition, either alone or in combination, contribute to the problem. This nonbeneficial gastrointestinal modulation may be reversed by judicious and controlled use of antibiotics and the appropriate use of prebiotics and probiotics. In certain persistent, recurrent settings, the option of faecal microbiota transplantation can be explored. The aim of the current review is to focus on the establishment and alteration of gut microbiota, with ageing. The review also discusses the potential role of gut microbiota in regulating the immune system, together with its function in healthy and diseased state.

Published

2018

216. Effects of life cycle and leaves location on gene expression and glycoside biosynthesis pathway in Stevia rebaudiana Bertoni.

Author

Ghaheri M, Adibrad E, Safavi SM, Kahrizi D, Soroush A, Muhammadi S, Ghorbani T, Sabzevari A, Ansarypour Z, and Rahmanian E

Subjects

Diterpenes, Kaurane analysis, Diterpenes, Kaurane genetics, Genes, Plant genetics, Glucosides analysis, Glucosides genetics, Stevia genetics, Stevia metabolism, Time Factors, Diterpenes, Kaurane biosynthesis, Gene Expression Regulation, Plant physiology, Glucosides biosynthesis, Life Cycle Stages physiology, Plant Leaves physiology, Stevia growth & development

Abstract

Stevia rebaudiana Bertoni is One of the most important biologically sourced and low-calorie sweeteners that known as "Sweet Weed". It contains steviol glycosides that they are about 200-300 times sweeter than sucrose. Tissue culture is the best method with high efficiency that can overcome to problems of traditional methods, and it is the most useful tools for studying stress tolerance mechanisms under in vitro conditions to obtain drought tolerance. In the present research, we investigated the impact of life cycle, leaves location and the harvesting time on expression of UGT74G1 and UGT76G1 as well as steviol glycosides accumulation. The highest gene expression of both UGT74G1 and UGT76G1 (207.677 and 208.396 Total Lab unit, respectively) was observed in young leaves in the second vegetative year. Also, the highest amount of stevioside accumulation (13.04) was due to the old leaves in vegetative stage which had significant differences with other effects whereas the lowest accumulation (7.47) was seen at young leaves at vegetative stage. Interestingly, the highest level of rebaudioside a production (15.74) was occurred at the young leaves at vegetative stage. There was significant differences between life cycle and leaves location on steviol glycoside production in stevia.

Published

2018

217. Relationship between visuospatial episodic memory, processing speed and executive function: are they stable over a lifespan?

Author

Dias BF, Rezende LO, Malloy-Diniz LF, and Paula JJ

Subjects

Adolescent, Adult, Age Factors, Aged, Aged, 80 and over, Aging physiology, Child, Female, Humans, Male, Mental Recall physiology, Middle Aged, Neuropsychological Tests, Reference Values, Time Factors, Young Adult, Cognition physiology, Executive Function physiology, Life Cycle Stages physiology, Memory, Episodic, Spatial Memory physiology

Abstract

The present study evaluated the association between episodic memory, executive function and processing speed in a sample with different age ranges. We tested the hypothesis that processing speed, executive function and memory are more strongly associated during childhood and old age. We evaluated 571 participants, aged six to 92 years, divided into four age groups: children/adolescents, young adults, middle-aged adults and older adults. Correlation analyses suggested that the shared variance between the processing speed and memory is strong in childhood but weak across other age ranges. Executive function, however, had a stronger association both in childhood and in old age, when compared with the intermediate stages. We conclude that the effects of processing speed and executive function on memory are not stable across human development. These functions may be compensatory mechanisms for memory functioning in childhood and old age.

Published

2018

218. Host and parasite thermal ecology jointly determine the effect of climate warming on epidemic dynamics.

Author

Gehman AM, Hall RJ, and Byers JE

Subjects

Acclimatization physiology, Animals, Climate Change, Ecology, Epidemics, Host-Parasite Interactions genetics, Life Cycle Stages physiology, Models, Biological, Temperature, Host-Parasite Interactions physiology, Hot Temperature adverse effects, Parasites physiology

Abstract

Host-parasite systems have intricately coupled life cycles, but each interactor can respond differently to changes in environmental variables like temperature. Although vital to predicting how parasitism will respond to climate change, thermal responses of both host and parasite in key traits affecting infection dynamics have rarely been quantified. Through temperature-controlled experiments on an ectothermic host-parasite system, we demonstrate an offset in the thermal optima for survival of infected and uninfected hosts and parasite production. We combine experimentally derived thermal performance curves with field data on seasonal host abundance and parasite prevalence to parameterize an epidemiological model and forecast the dynamical responses to plausible future climate-warming scenarios. In warming scenarios within the coastal southeastern United States, the model predicts sharp declines in parasite prevalence, with local parasite extinction occurring with as little as 2 °C warming. The northern portion of the parasite's current range could experience local increases in transmission, but assuming no thermal adaptation of the parasite, we find no evidence that the parasite will expand its range northward under warming. This work exemplifies that some host populations may experience reduced parasitism in a warming world and highlights the need to measure host and parasite thermal performance to predict infection responses to climate change., Competing Interests: The authors declare no conflict of interest.

Published

2018

219. Toward understanding barnacle cementing by characterization of one cement protein-100kDa in Amphibalanus amphitrite.

Author

He LS, Zhang G, Wang Y, Yan GY, and Qian PY

Subjects

Amino Acid Sequence, Animals, Molecular Sequence Data, Organ Specificity, Tissue Distribution, Adhesives chemistry, Adhesives metabolism, Arthropod Proteins chemistry, Arthropod Proteins metabolism, Life Cycle Stages physiology, Thoracica chemistry, Thoracica metabolism

Abstract

Barnacles, as major fouling organisms, have attracted more attentions. It is no doubt that the study on cement proteins is required to illustrate the mechanism of barnacle cementing. A cement protein defined as Aa-cp100k was characterized from Amphibalanus amphitrite in this study. The amino acid sequence of Aa-cp100k was shown a high similarity to other three barnacles including Megabalanus rosa (Mr-cp100k), Tetraclita japonica formosana (Tj-cp100k) and Pollicipes pollicipes (Pp-cp100k). Moreover, the localization of Aa-cp100k in the vacuoles of cyprid β secretory cells and the adult cement gland cells by immunofluorescence microscopy, indicating that Aa-cp100k existed in both cyprid and adult barnacle. Aa-cp100k from basal plate could be dissolved in urea buffer without high concentration of dithiothreitol (DTT), different from that in Megabalanus rosa, implying diverse possible roles of cp100k in cementing., (Copyright © 2017. Published by Elsevier Inc.)

Published

2018

220. Insights into the early liver stage biology of Plasmodium .

Author

Kori LD, Valecha N, and Anvikar AR

Subjects

Animals, Anopheles parasitology, Disease Models, Animal, Erythrocytes parasitology, Female, Humans, Liver cytology, Merozoites growth & development, Merozoites physiology, Mosquito Vectors parasitology, Plasmodium classification, Plasmodium genetics, Plasmodium growth & development, Sporozoites growth & development, Sporozoites physiology, Life Cycle Stages physiology, Liver parasitology, Plasmodium physiology

Abstract

Even though malaria is preventable and curable, it has become a serious threat to mankind. In 2016, there were an estimated 216 million cases of malaria across the world. The biology of its causative agent, i.e. Plasmodium parasite is full of complex mechanisms. There are five Plasmodium species responsible for malaria in humans, viz. Plasmodium falciparum, P. vivax, P. malariae, P. ovale and recently identified P. knowlesi that normally infect apes. In humans, malaria is spread by the injection of Plasmodium sporozoites through the bite of infectious Anopheles' female mosquito during their blood meal. From the time of entry into human skin till the development into the asexual forms, the parasite undergoes several transformations. This review attempts to understand the science behind the pre-erythrocytic liver stage of Plasmodium. Research articles explaining parasite biology, cell-traversal, transformation stages, cell-egress process, etc. were retrieved from PubMed and google scholar database. Various known and unknown mechanisms and strategies used by the malaria parasite P. berghei in rodent models have been discussed in this review. Limited or no information was available for humans, due to technical feasibility and complexity of parasite's life cycle. Hence, it was concluded that there is an urgent need to investigate the hepatic invasion, traversal and egress mechanism of P. falciparum and P. vivax for developing novel therapeutics to fight against malaria., Competing Interests: None

Published

2018

221. The role of particular ticks developmental stages in the circulation of tick-borne pathogens in Central Europe. 6. Babesia.

Author

Karbowiak G, Biernat B, Stańczak J, Werszko J, Szewczyk T, and Sytykiewicz H

Subjects

Animals, Europe epidemiology, Humans, Nymph, Rodentia parasitology, Babesia growth & development, Babesia physiology, Babesiosis epidemiology, Babesiosis parasitology, Babesiosis transmission, Ixodes parasitology, Life Cycle Stages physiology

Abstract

In the Central European conditions, three species of Babesia have epidemiological significance as human pathogens – Babesia divergens, B. microti and B. venatorum. Tick Ixodes ricinus is considered as their main vector, wild mammals as the animal reservoir. The zoonotic cycles of small and large Babesia differ in details. Due to the lack of transovarial mode transmission in small species B. microti, the circulation goes mainly between immature ticks and vertebrate hosts; pathogen circulates primarily in the cycle: infected rodent → the tick larva → the nymph → the mammal reservoir →the larva of the tick. The tick stages able to effectively infect human are nymphs and adult females, males do not participate in the follow transmission. For large Babesia – B. divergens and B. venatorum, the transovarial and transstadial transmission enable the presence of the agent in adult ticks, moreover, that larvae and nymphs feed on not-susceptible hosts. The tick stages able to effectively infect cattle and other ruminants are adult females. Resuming, pathogen circulates primarily in the cycle the ruminant host – adult female tick – the larva – the nymph – adult female of the next generation – the ruminant. Due to the compound developmental transmission has place after the outflow of a tick began feeding.

Published

2018

222. Amblyospora khaliulini (Microsporidia: Amblyosporidae): Investigations on its life cycle and ecology in Aedes communis (Diptera: Culicidae) and Acanthocyclops vernalis (Copepoda: Cyclopidae) with redescription of the species.

Author

Andreadis TG, Thomas MC, and Shepard JJ

Subjects

Animals, Host-Parasite Interactions physiology, Male, Aedes parasitology, Amblyospora growth & development, Copepoda parasitology, Culicidae parasitology, Life Cycle Stages physiology

Abstract

A multi-year study was conducted to examine the natural ecology of the microsporidium Amblyospora khaliulini and more fully characterize parasite development and histopathology in all stages of its primary mosquito host, Aedes communis and intermediate copepod host, Acanthocyclops vernalis with redescription of the species. A. khaliulini exhibits polymorphic development, produces three morphologically and functionally distinct spores, and is both horizontally and vertically transmitted. Development in A. vernalis is restricted to females, occurs within the ovaries and results in death of the host. Development is haplophasic with division by binary and multiple fission producing rosette-shaped sporogonial plasmodia and conical uninucleate spores that are orally infectious to Ae. communis larvae. Both sexes are equally susceptible and infections are confined to testes in males and ovaries in females. Initial stages of development include uninucleate schizonts that undergo karyokinesis forming diplokaryotic meronts that divide repeatedly by binary fission. Sporogony occurs in both host sexes, but sporogenesis does not progress normally in adult males and elliptical, thin walled binucleate spores that function in vertical transmission of the microsporidium via infection of the ovaries and eggs are formed in adult females only. Development of vertically acquired infections in larval Ae. communis hosts occurs within fat body tissue, leads to the production of meiospores in male hosts only and results in death during the 4th larval stadium. Initial development is characterized by merogonial multiplication of diplokarya by synchronous binary division producing additional diplokarya. The cessation of merogony and the onset of sporogony are characterized by the simultaneous secretion of a sporophorous vesicle and meiotic division of diplokarya resulting in the formation of octonucleate sporonts that undergo cytokinesis and sporogenesis to form eight uninucleate, broadly ovoid meiospores enclosed within a sporophorous vesicle. The natural prevalence of patent vertically acquired fat body infections in field populations of Ae. communis ranged from 1.6% to 3.6%. Yearly infection rates in A. vernalis copepods ranged from 57.1% to 15.0%. Prevalence rates of horizontally acquired infections in emerging adult Ae. communis ranged from 69.0% to 11.9% in males and 50.0% to 16.4% in females., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2018

223. Temperature fine-tunes Mediterranean Arabidopsis thaliana life-cycle phenology geographically.

Author

Marcer A, Vidigal DS, James PMA, Fortin MJ, Méndez-Vigo B, Hilhorst HWM, Bentsink L, Alonso-Blanco C, and Picó FX

Subjects

Arabidopsis genetics, Arabidopsis growth & development, Flowers growth & development, Flowers physiology, Genetic Variation genetics, Genetic Variation physiology, Geography, Life Cycle Stages physiology, Mediterranean Region, Phenotype, Plant Dormancy genetics, Plant Dormancy physiology, Arabidopsis physiology, Temperature

Abstract

To understand how adaptive evolution in life-cycle phenology operates in plants, we need to unravel the effects of geographic variation in putative agents of natural selection on life-cycle phenology by considering all key developmental transitions and their co-variation patterns. We address this goal by quantifying the temperature-driven and geographically varying relationship between seed dormancy and flowering time in the annual Arabidopsis thaliana across the Iberian Peninsula. We used data on genetic variation in two major life-cycle traits, seed dormancy (DSDS50) and flowering time (FT), in a collection of 300 A. thaliana accessions from the Iberian Peninsula. The geographically varying relationship between life-cycle traits and minimum temperature, a major driver of variation in DSDS50 and FT, was explored with geographically weighted regressions (GWR). The environmentally varying correlation between DSDS50 and FT was analysed by means of sliding window analysis across a minimum temperature gradient. Maximum local adjustments between minimum temperature and life-cycle traits were obtained in the southwest Iberian Peninsula, an area with the highest minimum temperatures. In contrast, in off-southwest locations, the effects of minimum temperature on DSDS50 were rather constant across the region, whereas those of minimum temperature on FT were more variable, with peaks of strong local adjustments of GWR models in central and northwest Spain. Sliding window analysis identified a minimum temperature turning point in the relationship between DSDS50 and FT around a minimum temperature of 7.2 °C. Above this minimum temperature turning point, the variation in the FT/DSDS50 ratio became rapidly constrained and the negative correlation between FT and DSDS50 did not increase any further with increasing minimum temperatures. The southwest Iberian Peninsula emerges as an area where variation in life-cycle phenology appears to be restricted by the duration and severity of the hot summer drought. The temperature-driven varying relationship between DSDS50 and FT detected environmental boundaries for the co-evolution between FT and DSDS50 in A. thaliana. In the context of global warming, we conclude that A. thaliana phenology from the southwest Iberian Peninsula, determined by early flowering and deep seed dormancy, might become the most common life-cycle phenotype for this annual plant in the region., (© 2017 German Botanical Society and The Royal Botanical Society of the Netherlands.)

Published

2018

224. The Arboranan Frogs: Introduction.

Author

Schmid M, Steinlein C, Haaf T, Feightinger W, Guttenbach M, Bogart JP, Gruber SL, Kasahara S, Kakampuy W, Del Pino EM, Carrillo AB, Romero-Carvajal A, Mahony M, King M, Duellman WE, and Hedges SB

Subjects

Animals, Female, Life Cycle Stages physiology, Male, Oogenesis physiology, Phylogeny, Phylogeography, Ranidae anatomy & histology, Ranidae genetics, Ranidae growth & development, Spermatogenesis physiology, Terminology as Topic, Animal Distribution physiology, Biological Evolution, Ranidae classification

Published

2018

225. PvaxDB: a comprehensive structural repository of Plasmodium vivax proteome.

Author

Singh A, Kaushik R, Kuntal H, and Jayaram B

Subjects

Humans, Databases, Protein, Life Cycle Stages physiology, Malaria, Vivax genetics, Malaria, Vivax metabolism, Plasmodium vivax genetics, Plasmodium vivax growth & development, Plasmodium vivax metabolism, Protozoan Proteins genetics, Protozoan Proteins metabolism

Abstract

Database Url: http://www.scfbio-iitd.res.in/PvaxDB.

Published

2018

226. Biology of the introduced species Triatoma lecticularia (Hemiptera: Reduviidae) to northwestern Mexico, under laboratory conditions.

Author

Grant-Guillén Y, Nogueda-Torres B, Gascón-Sánchez J, Goicochea-Del Rosal G, and Martínez-Ibarra JA

Subjects

Animals, Disease Vectors, Humans, Mexico, Chagas Disease transmission, Feeding Behavior physiology, Insect Vectors physiology, Introduced Species, Life Cycle Stages physiology, Nymph physiology, Triatoma growth & development

Abstract

The first record of Triatoma lecticularia out of its reported distribution area together with the brief description of the said area is provided in this paper. In addition, some biological parameters related to hatching of eggs, life cycle and feeding and defecation behaviors for each instar of one population of T. lecticularia from its previously reported distribution area (PR) and for each instar of that introduced recently found population (IS) of this species were evaluated and compared. Twenty-eight specimens were collected from IS, mostly (64.29%) from peridomestic areas (mainly chicken coops). No significant (p>0.05) differences were recorded between the two studied cohorts in their average time to hatch, which was close to 19days. The median egg-to-adult development time, the number of blood meals at each nymphal, the instar mortality rates and median time-lapse for beginning of feeding were significantly (p<0.05) shorter for the IS cohort. Median feeding time was higher in PR. Defecation delay was shorter than 10min in both studied cohorts. Given these results, the introduced recently found population of T. lecticularia could be considered an important potential vector of Trypanosoma cruzi to human populations and could replace main triatomine species on its new distribution area., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2018

227. A paradigm shift: The mitoproteomes of procyclic and bloodstream Trypanosoma brucei are comparably complex.

Author

Zíková A, Verner Z, Nenarokova A, Michels PAM, and Lukeš J

Subjects

Animals, Humans, Life Cycle Stages physiology, Proteome analysis, Proteome metabolism, Mitochondrial Proteins metabolism, Protozoan Proteins metabolism, Trypanosoma brucei brucei growth & development, Trypanosoma brucei brucei metabolism

Published

2017

228. Identification and characterization of the three members of the CLC family of anion transport proteins in Trypanosoma brucei.

Author

Steinmann ME, Schmidt RS, Macêdo JP, Kunz Renggli C, Bütikofer P, Rentsch D, Mäser P, and Sigel E

Subjects

4,4'-Diisothiocyanostilbene-2,2'-Disulfonic Acid pharmacology, Animals, Chloride Channels antagonists & inhibitors, Chloride Channels metabolism, Chlorides metabolism, Endoplasmic Reticulum ultrastructure, Female, Gene Expression, Genetic Complementation Test, Golgi Apparatus metabolism, Golgi Apparatus ultrastructure, Humans, Ion Transport, Membrane Potentials drug effects, Membrane Potentials physiology, Nitrates metabolism, Oocytes cytology, Oocytes drug effects, Oocytes metabolism, Patch-Clamp Techniques, Protein Multimerization, Protozoan Proteins antagonists & inhibitors, Protozoan Proteins metabolism, Saccharomyces cerevisiae genetics, Trypanosoma brucei brucei growth & development, Trypanosoma brucei brucei ultrastructure, Xenopus laevis, Chloride Channels genetics, Endoplasmic Reticulum metabolism, Life Cycle Stages physiology, Protozoan Proteins genetics, Saccharomyces cerevisiae metabolism, Trypanosoma brucei brucei metabolism

Abstract

CLC type anion transport proteins are homo-dimeric or hetero-dimeric with an integrated transport function in each subunit. We have identified and partially characterized three members of this family named TbVCL1, TbVCL2 and TbVCL3 in Trypanosoma brucei. Among the human CLC family members, the T. brucei proteins display highest similarity to CLC-6 and CLC-7. TbVCL1, but not TbVCL2 and TbVCL3 is able to complement growth of a CLC-deficient Saccharomyces cerevisiae mutant. All TbVCL-HA fusion proteins localize intracellulary in procyclic form trypanosomes. TbVCL1 localizes close to the Golgi apparatus and TbVCL2 and TbVCL3 to the endoplasmic reticulum. Upon expression in Xenopus oocytes, all three proteins induce similar outward rectifying chloride ion currents. Currents are sensitive to low concentrations of DIDS, insensitive to the pH in the range 5.4 to 8.4 and larger in nitrate than in chloride medium.

Published

2017

229. Systematic CRISPR-Cas9-Mediated Modifications of Plasmodium yoelii ApiAP2 Genes Reveal Functional Insights into Parasite Development.

Author

Zhang C, Li Z, Cui H, Jiang Y, Yang Z, Wang X, Gao H, Liu C, Zhang S, Su XZ, and Yuan J

Subjects

Animals, Female, Gene Knockout Techniques, Life Cycle Stages physiology, Malaria parasitology, Male, Mice, Oocysts genetics, Oocysts metabolism, Plasmodium yoelii growth & development, Plasmodium yoelii physiology, Sporozoites genetics, Sporozoites metabolism, CRISPR-Cas Systems genetics, Gene Expression Regulation, Life Cycle Stages genetics, Plasmodium yoelii genetics, Protozoan Proteins genetics

Abstract

Malaria parasites have a complex life cycle with multiple developmental stages in mosquito and vertebrate hosts, and different developmental stages express unique sets of genes. Unexpectedly, many transcription factors (TFs) commonly found in eukaryotic organisms are absent in malaria parasites; instead, a family of genes encoding proteins similar to the plant Apetala2 (ApiAP2) transcription factors is expanded in the parasites. Several malaria ApiAP2 genes have been shown to play a critical role in parasite development; however, the functions of the majority of the ApiAP2 genes remain to be elucidated. In particular, no study on the Plasmodium yoelii ApiAP2 (PyApiAP2) gene family has been reported so far. This study systematically investigated the functional roles of PyApiAP2 genes in parasite development. Twenty-four of the 26 PyApiAP2 genes were selected for disruption, and 12 were successfully knocked out using the clustered regularly interspaced short palindromic repeat-CRISPR-associated protein 9 (CRISPR-Cas9) method. The effects of gene knockout (KO) on parasite development in mouse and mosquito stages were evaluated. Ten of 12 successfully disrupted genes, including two genes that have not been functionally characterized in any Plasmodium species previously, were shown to be critical for P. yoelii development of sexual and mosquito stages. Additionally, seven of the genes were labeled for protein expression analysis, revealing important information supporting their functions. This study represents the first systematic functional characterization of the P. yoelii ApiAP2 gene family and discovers important insights on the roles of the ApiAP2 genes in parasite development. IMPORTANCE Malaria is a parasitic disease that infects hundreds of millions of people, leading to an estimated 0.35 million deaths in 2015. A better understanding of the mechanism of gene expression regulation during parasite development may provide important clues for disease control and prevention. In this study, systematic gene disruption experiments were performed to study the functional roles of members of the Plasmodium yoelii ApiAP2 (PyApiAP2) gene family in parasite development. Genes that are critical for the development of male and female gametocytes, oocysts, and sporozoites were characterized. The protein expression profiles for seven of the PyApiAP2 gene products were also analyzed, revealing important information on their functions. This study provides expression and functional information for many PyApiAP2 genes, which can be explored for disease management.

Published

2017

230. Translational Control in the Latency of Apicomplexan Parasites.

Author

Holmes MJ, Augusto LDS, Zhang M, Wek RC, and Sullivan WJ Jr

Subjects

Apicomplexa genetics, Host-Parasite Interactions genetics, Humans, Life Cycle Stages genetics, Phosphorylation, Protozoan Proteins genetics, Apicomplexa physiology, Eukaryotic Initiation Factor-2 metabolism, Host-Parasite Interactions physiology, Life Cycle Stages physiology, Protozoan Proteins metabolism, Transcriptome

Abstract

Apicomplexan parasites Toxoplasma gondii and Plasmodium spp. use latent stages to persist in the host, facilitate transmission, and thwart treatment of infected patients. Therefore, it is important to understand the processes driving parasite differentiation to and from quiescent stages. Here, we discuss how a family of protein kinases that phosphorylate the eukaryotic initiation factor-2 (eIF2) function in translational control and drive differentiation. This translational control culminates in reprogramming of the transcriptome to facilitate parasite transition towards latency. We also discuss how eIF2 phosphorylation contributes to the maintenance of latency and provides a crucial role in the timing of reactivation of latent parasites towards proliferative stages., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

231. Non-parasitic life cycle of the cattle tick Rhipicephalus (Boophilus) microplus in Panicum maximum pastures in northern Argentina.

Author

Mastropaolo M, Mangold AJ, Guglielmone AA, and Nava S

Subjects

Animals, Argentina, Female, Larva, Oviposition, Ovum, Seasons, Time Factors, Life Cycle Stages physiology, Panicum, Rhipicephalus physiology

Abstract

The aim of this work was to study the non-parasitic phase of the Rhipicephalus microplus life cycle in Panicum maximum grasses from northern Argentina, in order to provide ecological information for designing methods of tick control. Four localities were chosen as replicates. The biological parameters measured were proportion of females ovipositing, the pre-oviposition period, the proportion of egg clusters hatching, the incubation period of eggs, larval longevity, and the total non-parasitic period (time from the exposure of the female to the date of death of the last larva) (TNPP)). The following general trends were observed: I) a longer TNPP occurred when female ticks were exposed in mid- and late summer and early spring; II) the shortest TNPP occurred when female ticks were exposed from late winter to late spring; III) larvae that were active in early and mid-summer had the shortest longevity; IV) incubation periods of eggs, which originated from females exposed in late summer, early autumn and mid-spring, were longer than the incubation period of eggs produced by females exposed in late spring and early summer; V) eggs did not hatch when the engorged females were exposed in the pastures in mid- and late autumn and winter. The spelling period of the P. maximum grasses that is needed to ensure total control of R. microplus consists of 19-20weeks if the spelling starts in late spring and early summer, and 27-28weeks if the spelling begins in mid- and late summer or in autumn., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

232. Fragmentation modes and the evolution of life cycles.

Author

Pichugin Y, Peña J, Rainey PB, and Traulsen A

Subjects

Animals, Bacteria cytology, Computational Biology, Reproduction physiology, Biological Evolution, Cell Physiological Phenomena physiology, Life Cycle Stages physiology, Models, Biological

Abstract

Reproduction is a defining feature of living systems. To reproduce, aggregates of biological units (e.g., multicellular organisms or colonial bacteria) must fragment into smaller parts. Fragmentation modes in nature range from binary fission in bacteria to collective-level fragmentation and the production of unicellular propagules in multicellular organisms. Despite this apparent ubiquity, the adaptive significance of fragmentation modes has received little attention. Here, we develop a model in which groups arise from the division of single cells that do not separate but stay together until the moment of group fragmentation. We allow for all possible fragmentation patterns and calculate the population growth rate of each associated life cycle. Fragmentation modes that maximise growth rate comprise a restrictive set of patterns that include production of unicellular propagules and division into two similar size groups. Life cycles marked by single-cell bottlenecks maximise population growth rate under a wide range of conditions. This surprising result offers a new evolutionary explanation for the widespread occurrence of this mode of reproduction. All in all, our model provides a framework for exploring the adaptive significance of fragmentation modes and their associated life cycles.

Published

2017

233. Ardissonea crystallina has a type of sexual reproduction that is unusual for centric diatoms.

Author

Davidovich NA, Davidovich OI, Podunay YA, Gastineau R, Kaczmarska I, Poulíčková A, and Witkowski A

Subjects

Diatoms genetics, Diatoms ultrastructure, Germ Cells physiology, Germ Cells ultrastructure, Life Cycle Stages physiology, Microscopy, Electron, Scanning, Phylogeny, Reproduction physiology, Diatoms physiology

Abstract

Molecular phylogenetic analyses place Ardissonea crystallina (C. Agardh) Grunow and all Toxariids among the bi- and multipolar centric diatoms, almost always recovered as a derived lineage sister to Lampriscus. In all centrics where sexual reproduction has been documented, oogamy, with larger immobile eggs and smaller flagellated sperm has been observed. We were able to initiate both homothallic and heterothallic reproduction in A. crystallina. The heterothallic reproduction turned out to be non-oogamous; gametes were more or less equal in size but no flagellated cells were detected. At the same time, two mating types ("male" and "female") were recognized by the distinct morphology and behaviour of the gametes. While no flagella were observed, periodically thin cytoplasmic projections arose on the surface of the "male" gametes. These projections similar to those found in some pennate diatoms facilitated contact with the "female" cells. In each gametangial cell, regardless of the mating type, only one gamete was formed. Thus, the Toxariids may represent a unique evolutionary group, at least in respect to their reproductive biology. The hypothesis discussed is that non-oogamous mode of reproduction could have evolved in Ardissonea (and possibly in other Toxariids) independently of the pennate lineage of diatoms.

Published

2017

234. The regulation of autophagy differentially affects Trypanosoma cruzi metacyclogenesis.

Author

Vanrell MC, Losinno AD, Cueto JA, Balcazar D, Fraccaroli LV, Carrillo C, and Romano PS

Subjects

Adult, Animals, Autophagosomes parasitology, Cell Differentiation, Chagas Disease parasitology, Humans, Life Cycle Stages physiology, Male, Polyamines metabolism, Spermidine metabolism, Stress, Physiological, Trypanosoma cruzi genetics, Autophagy, Gene Expression Regulation, Life Cycle Stages genetics, Protozoan Proteins genetics, Trypanosoma cruzi physiology

Abstract

Autophagy is a cellular process required for the removal of aged organelles and cytosolic components through lysosomal degradation. All types of eukaryotic cells from yeasts to mammalian cells have the machinery to activate autophagy as a result of many physiological and pathological situations. The most frequent stimulus of autophagy is starvation and the result, in this case, is the fast generation of utilizable food (e.g. amino acids and basic nutrients) to maintain the vital biological processes. In some organisms, starvation also triggers other associated processes such as differentiation. The protozoan parasite Trypanosoma cruzi undergoes a series of differentiation processes throughout its complex life cycle. Although not all autophagic genes have been identified in the T. cruzi genome, previous works have demonstrated the presence of essential autophagic-related proteins. Under starvation conditions, TcAtg8, which is the parasite homolog of Atg8/LC3 in other organisms, is located in autophagosome-like vesicles. In this work, we have characterized the autophagic pathway during T. cruzi differentiation from the epimastigote to metacyclic trypomastigote form, a process called metacyclogenesis. We demonstrated that autophagy is stimulated during metacyclogenesis and that the induction of autophagy promotes this process. Moreover, with exception of bafilomycin, other classical autophagy modulators have similar effects on T. cruzi autophagy. We also showed that spermidine and related polyamines can positively regulate parasite autophagy and differentiation. We concluded that both polyamine metabolism and autophagy are key processes during T. cruzi metacyclogenesis that could be exploited as drug targets to avoid the parasite cycle progression.

Published

2017

235. Compositional and expression analyses of the glideosome during the Plasmodium life cycle reveal an additional myosin light chain required for maximum motility.

Author

Green JL, Wall RJ, Vahokoski J, Yusuf NA, Ridzuan MAM, Stanway RR, Stock J, Knuepfer E, Brady D, Martin SR, Howell SA, Pires IP, Moon RW, Molloy JE, Kursula I, Tewari R, and Holder AA

Subjects

Animals, Humans, Mice, Life Cycle Stages physiology, Membrane Proteins genetics, Membrane Proteins metabolism, Myosins genetics, Myosins metabolism, Plasmodium berghei genetics, Plasmodium berghei metabolism, Plasmodium falciparum genetics, Plasmodium falciparum metabolism, Protozoan Proteins genetics, Protozoan Proteins metabolism

Abstract

Myosin A (MyoA) is a Class XIV myosin implicated in gliding motility and host cell and tissue invasion by malaria parasites. MyoA is part of a membrane-associated protein complex called the glideosome, which is essential for parasite motility and includes the MyoA light chain myosin tail domain-interacting protein (MTIP) and several glideosome-associated proteins (GAPs). However, most studies of MyoA have focused on single stages of the parasite life cycle. We examined MyoA expression throughout the Plasmodium berghei life cycle in both mammalian and insect hosts. In extracellular ookinetes, sporozoites, and merozoites, MyoA was located at the parasite periphery. In the sexual stages, zygote formation and initial ookinete differentiation precede MyoA synthesis and deposition, which occurred only in the developing protuberance. In developing intracellular asexual blood stages, MyoA was synthesized in mature schizonts and was located at the periphery of segmenting merozoites, where it remained throughout maturation, merozoite egress, and host cell invasion. Besides the known GAPs in the malaria parasite, the complex included GAP40, an additional myosin light chain designated essential light chain (ELC), and several other candidate components. This ELC bound the MyoA neck region adjacent to the MTIP-binding site, and both myosin light chains co-located to the glideosome. Co-expression of MyoA with its two light chains revealed that the presence of both light chains enhances MyoA-dependent actin motility. In conclusion, we have established a system to study the interplay and function of the three glideosome components, enabling the assessment of inhibitors that target this motor complex to block host cell invasion., (© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2017

236. Black Truffle, a Hermaphrodite with Forced Unisexual Behaviour.

Author

Selosse MA, Schneider-Maunoury L, Taschen E, Rousset F, and Richard F

Subjects

DNA, Fungal genetics, Life Cycle Stages genetics, Life Cycle Stages physiology, Soil Microbiology, Ascomycota genetics, Ascomycota physiology

Abstract

The life cycle of the black truffle (Tuber melanosporum) includes a mating before sporulation: although the species is hermaphroditic, mating turns out to involve parents with very different features, that mostly behave as male or female only, suggesting that this species undergoes forced dioecism., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

237. An Integrated Approach to Explore Composition and Dynamics of Cholesterol-rich Membrane Microdomains in Sexual Stages of Malaria Parasite.

Author

Fratini F, Raggi C, Sferra G, Birago C, Sansone A, Grasso F, Currà C, Olivieri A, Pace T, Mochi S, Picci L, Ferreri C, Di Biase A, Pizzi E, and Ponzi M

Subjects

Animals, Cholesterol chemistry, Cholesterol metabolism, Computer Simulation, Detergents chemistry, Disease Models, Animal, Gametogenesis physiology, Humans, Lipids analysis, Membrane Microdomains chemistry, Mice, Mice, Inbred BALB C, Proteomics, Sphingolipids chemistry, Sphingolipids metabolism, Life Cycle Stages physiology, Malaria parasitology, Membrane Microdomains metabolism, Plasmodium berghei growth & development, Plasmodium berghei metabolism

Abstract

Membrane microdomains that include lipid rafts, are involved in key physiological and pathological processes and participate in the entry of endocellular pathogens. These assemblies, enriched in cholesterol and sphingolipids, form highly dynamic, liquid-ordered phases that can be separated from the bulk membranes thanks to their resistance to solubilization by nonionic detergents. To characterize complexity and dynamics of detergent-resistant membranes of sexual stages of the rodent malaria parasite Plasmodium berghei , here we propose an integrated study of raft components based on proteomics, lipid analysis and bioinformatics. This analysis revealed unexpected heterogeneity and unexplored pathways associated with these specialized assemblies. Protein-protein relationships and protein-lipid co-occurrence were described through multi-component networks. The proposed approach can be widely applied to virtually every cell type in different contexts and perturbations, under physiological and/or pathological conditions., (© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2017

238. Sleeper cells: the stringent response and persistence in the Borreliella (Borrelia) burgdorferi enzootic cycle.

Author

Cabello FC, Godfrey HP, Bugrysheva JV, and Newman SA

Subjects

Animals, Anti-Bacterial Agents therapeutic use, Borrelia burgdorferi drug effects, Drug Resistance, Multiple, Bacterial, Europe, Humans, Lyme Disease microbiology, Mice, North America, Borrelia burgdorferi growth & development, Borrelia burgdorferi pathogenicity, Ixodes microbiology, Life Cycle Stages physiology, Lyme Disease pathology

Abstract

Infections with tick-transmitted Borreliella (Borrelia) burgdorferi, the cause of Lyme disease, represent an increasingly large public health problem in North America and Europe. The ability of these spirochetes to maintain themselves for extended periods of time in their tick vectors and vertebrate reservoirs is crucial for continuance of the enzootic cycle as well as for the increasing exposure of humans to them. The stringent response mediated by the alarmone (p)ppGpp has been determined to be a master regulator in B. burgdorferi. It modulates the expression of identified and unidentified open reading frames needed to deal with and overcome the many nutritional stresses and other challenges faced by the spirochete in ticks and animal reservoirs. The metabolic and morphologic changes resulting from activation of the stringent response in B. burgdorferi may also be involved in the recently described non-genetic phenotypic phenomenon of tolerance to otherwise lethal doses of antimicrobials and to other antimicrobial activities. It may thus constitute a linchpin in multiple aspects of infections with Lyme disease borrelia, providing a link between the micro-ecological challenges of its enzootic life-cycle and long-term residence in the tissues of its animal reservoirs, with the evolutionary side effect of potential persistence in incidental human hosts., (© 2017 Society for Applied Microbiology and John Wiley & Sons Ltd.)

Published

2017

239. Evidence for complex life cycle constraints on salamander body form diversification.

Author

Bonett RM and Blair AL

Subjects

Animals, Biological Evolution, Body Size, Ecology, Larva anatomy & histology, Larva physiology, Metamorphosis, Biological, Phenotype, Phylogeny, Life Cycle Stages physiology, Urodela growth & development, Urodela physiology

Abstract

Metazoans display a tremendous diversity of developmental patterns, including complex life cycles composed of morphologically disparate stages. In this regard, the evolution of life cycle complexity promotes phenotypic diversity. However, correlations between life cycle stages can constrain the evolution of some structures and functions. Despite the potential macroevolutionary consequences, few studies have tested the impacts of life cycle evolution on broad-scale patterns of trait diversification. Here we show that larval and adult salamanders with a simple, aquatic-only (paedomorphic) life cycle had an increased rate of vertebral column and body form diversification compared to lineages with a complex, aquatic-terrestrial (biphasic) life cycle. These differences in life cycle complexity explain the variations in vertebral number and adult body form better than larval ecology. In addition, we found that lineages with a simple terrestrial-only (direct developing) life cycle also had a higher rate of adult body form evolution than biphasic lineages, but still 10-fold lower than aquatic-only lineages. Our analyses demonstrate that prominent shifts in phenotypic evolution can follow long-term transitions in life cycle complexity, which may reflect underlying stage-dependent constraints., Competing Interests: The authors declare no conflict of interest.

Published

2017

240. The Toxoplasma gondii inhibitor-2 regulates protein phosphatase 1 activity through multiple motifs.

Author

Deveuve Q, Lesage K, Mouveaux T, and Gissot M

Subjects

Amino Acid Sequence, Animals, Cat Diseases parasitology, Cats, Cloning, Molecular, Humans, Life Cycle Stages physiology, Okadaic Acid pharmacology, Phosphorylation physiology, Protein Phosphatase 1 genetics, Protein Phosphatase 1 metabolism, Proteins genetics, Protein Phosphatase 1 antagonists & inhibitors, Proteins metabolism, Toxoplasma physiology

Abstract

Toxoplasma gondii has a complex life cycle characterized by multiple differentiation steps that are essential for its survival in both human and definitive feline host. Several studies have demonstrated the importance of phosphorylations by protein kinases during the life cycle of T. gondii. However, very little is known about protein phosphatases and their regulators in the parasite. We report the molecular and functional characterization of the T. gondii ortholog of the inhibitor-2 protein, designated TgI2. We show that TgI2 encompasses conserved motifs involved in the interaction and modulation of the phosphatase activity of T. gondii protein phosphatase 1, named TgPP1. We show that a specific combination of motifs is involved in binding and/or inhibition of the TgPP1 activity. We show here that the TgI2 protein is a potent inhibitor of TgPP1 phosphatase activity. TgI2 SILK and RVxF motifs are critical for regulating the activity of TgPP1, a feature that is common with the higher eukaryotes inhibitor-2 protein.

Published

2017

241. Shape, form, function and Leishmania pathogenicity: from textbook descriptions to biological understanding.

Author

Sunter J and Gull K

Subjects

Animals, Flagella physiology, Flagella ultrastructure, Humans, Leishmania ultrastructure, Leishmaniasis, Cutaneous parasitology, Leishmaniasis, Cutaneous pathology, Leishmaniasis, Visceral parasitology, Leishmaniasis, Visceral pathology, Macrophages parasitology, Macrophages pathology, Phlebotomus parasitology, Psychodidae parasitology, Insect Vectors parasitology, Leishmania growth & development, Leishmania pathogenicity, Leishmaniasis, Cutaneous transmission, Leishmaniasis, Visceral transmission, Life Cycle Stages physiology

Abstract

The shape and form of protozoan parasites are inextricably linked to their pathogenicity. The evolutionary pressure associated with establishing and maintaining an infection and transmission to vector or host has shaped parasite morphology. However, there is not a 'one size fits all' morphological solution to these different pressures, and parasites exhibit a range of different morphologies, reflecting the diversity of their complex life cycles. In this review, we will focus on the shape and form of Leishmania spp., a group of very successful protozoan parasites that cause a range of diseases from self-healing cutaneous leishmaniasis to visceral leishmaniasis, which is fatal if left untreated., (© 2017 The Authors.)

Published

2017

242. Life-span of in vitro differentiated Plasmodium falciparum gametocytes.

Author

Gebru T, Lalremruata A, Kremsner PG, Mordmüller B, and Held J

Subjects

Flow Cytometry, In Vitro Techniques, Longevity, Microscopy, Plasmodium falciparum genetics, Polymerase Chain Reaction, Life Cycle Stages physiology, Plasmodium falciparum growth & development

Abstract

Background: The sexual stages (gametocytes) of Plasmodium falciparum do not directly contribute to the pathology of malaria but are essential for transmission of the parasite from the human host to the mosquito. Mature gametocytes circulate in infected human blood for several days and their circulation time has been modelled mathematically from data of previous in vivo studies. This is the first time that longevity of gametocytes is studied experimentally in vitro., Methods: The in vitro longevity of P. falciparum gametocytes of 1 clinical isolate and 2 laboratory strains was assessed by three different methods: microscopy, flow cytometry and reverse transcription quantitative real-time PCR (RT-qPCR). Additionally, the rate of gametocytogenesis of the used P. falciparum strains was compared., Results: The maximum in vitro lifespan of P. falciparum gametocytes reached almost 2 months (49 days by flow cytometry, 46 days by microscopy, and at least 52 days by RT-qPCR) from the starting day of gametocyte culture to death of last parasite in the tested strains with an average 50% survival rate of 6.5, 2.6 and 3.5 days, respectively. Peak gametocytaemia was observed on average 19 days after initiation of gametocyte culture followed by a steady decline due to natural decay of the parasites. The rate of gametocytogenesis was highest in the NF54 strain., Conclusions: Plasmodium falciparum mature gametocytes can survive up to 16-32 days (at least 14 days for mature male gametocytes) in vitro in absence of the influence of host factors. This confirms experimentally a previous modelling estimate that used molecular tools for gametocyte detection in treated patients. The survival time might reflect the time the parasite can be transmitted to the mosquito after clearance of asexual parasites. These results underline the importance of efficient transmission blocking agents in the fight against malaria.

Published

2017

243. Insights on Heme Synthesis in the Malaria Parasite.

Author

Nagaraj VA and Padmanaban G

Subjects

Animals, Culicidae parasitology, Heme genetics, Heme metabolism, Humans, Life Cycle Stages physiology, Plasmodium falciparum genetics, Heme biosynthesis, Host-Pathogen Interactions, Plasmodium falciparum metabolism

Abstract

The malaria parasite has a functional heme-biosynthetic pathway, although it can access host hemoglobin-heme. The heme pathway is dispensable for blood stages, but essential in the mosquito stages which do not acquire hemoglobin-heme. We propose that the blood stage parasites maintain a dynamic heme pool through multiple back-up mechanisms., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

244. Colder is better: The differential effects of thermal acclimation on life history parameters in a parasitoid fly.

Author

Zamorano J, Bozinovic F, and Veloso C

Subjects

Acclimatization physiology, Animals, Female, Life Cycle Stages physiology, Male, Random Allocation, Reproduction physiology, Survival Analysis, Time Factors, Diptera physiology, Temperature

Abstract

In this article, we assessed the effect of the rearing temperature on life history traits of the poorly known fly Phasmovora phasmophagae (Diptera: Tachinidae), a parasitoid of Agathemera crassa (Phasmatodea: Agathemeridae) in order to: i) test the effect of ambient temperature on life history traits and ii) assess the potential trade-off between reproduction and survival. Parasitoids were obtained from a population of hosts located in the Andes range of central Chile. Upon emergence from the host parasitoids were randomly allocated to three thermal treatments (15°C, 22.5°C and 30°C) and several life history traits were measured. We recorded higher survival at 15°C and 22.5°C and a lower survival at 30°C.We found differences for both body mass and head width among thermal treatments. In females, body mass was higher at 15°C than at 30°C. An effect of breeding temperature and sex was observed only for developmental time. In addition, males reared at different temperatures during the pupal stage and held as adults at 22.5°C, exhibited no differences in longevity between treatments. A significant effect of temperature on the mass of ovaries and lipid was recorded in females. These patterns suggest a trade-off between reproduction and survival. Overall, data seem to support the "colder is better" hypothesis, because Andean parasitoid P. phasmophagae inhabiting and experimentally reared in colder environments have a higher performance in all environments., (Copyright © 2017. Published by Elsevier Ltd.)

Published

2017

245. Synergistic blending of high-valued heterocycles inhibits growth of Plasmodium falciparum in culture and P. berghei infection in mouse model.

Author

Kumar P, Achieng AO, Rajendran V, Ghosh PC, Singh BK, Rawat M, Perkins DJ, Kempaiah P, and Rathi B

Subjects

Animals, Antimalarials chemical synthesis, Artemisinins pharmacology, Chloroquine pharmacology, Disease Models, Animal, Drug Synergism, Drug Therapy, Combination, Erythrocytes drug effects, Erythrocytes parasitology, Female, Humans, Inhibitory Concentration 50, Life Cycle Stages physiology, Malaria parasitology, Mice, Phthalimides chemical synthesis, Plasmodium berghei growth & development, Plasmodium falciparum growth & development, Antimalarials pharmacology, Life Cycle Stages drug effects, Malaria drug therapy, Phthalimides pharmacology, Plasmodium berghei drug effects, Plasmodium falciparum drug effects

Abstract

A series of phthalimide analogues, novelized with high-valued bioactive scaffolds was synthesized by means of click-chemistry under non-conventional microwave heating and evaluated as noteworthy growth inhibitors of Plasmodium falciparum (3D7 and W2) in culture. Analogues 6a, 6h and 6 u showed highest activity to inhibit the growth of the parasite with IC 50 values in submicromolar range. Structure-activity correlation indicated the necessity of unsubstituted triazoles and leucine linker to obtain maximal growth inhibition of the parasite. Notably, phthalimide 6a and 6u selectively inhibited the ring-stage growth and parasite maturation. On other hand, phthalimide 6h displayed selective schizonticidal activity. Besides, they displayed synergistic interactions with chloroquine and dihydroartemisinin against parasite. Additional in vivo experiments using P. berghei infected mice showed that administration of 6h and 6u alone, as well as in combination with dihydroartemisinin, substantially reduced the parasite load. The high antimalarial activity of 6h and 6u, coupled with low toxicity advocate their potential role as novel antimalarial agents, either as standalone or combination therapies.

Published

2017

246. Malaria Eradication and the Hidden Parasite Reservoir.

Author

Markus MB

Subjects

Animals, Bone Marrow Cells parasitology, Humans, Life Cycle Stages physiology, Malaria prevention & control, Recurrence, Spleen parasitology, Carrier State parasitology, Disease Eradication, Erythrocytes parasitology, Malaria parasitology, Plasmodium vivax physiology

Abstract

Accumulation of erythrocytic parasites in bone marrow and the spleen has been reported in cases of Plasmodium vivax malaria. If this occurs commonly, these stages represent a possible source of early, relapse-like homologous recurrences. Moreover, they might hinder the elimination of malaria from human populations. Pertinent research suggestions have been made., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

247. Impact of constant versus fluctuating temperatures on the development and life history parameters of Tetranychus urticae (Acari: Tetranychidae).

Author

Bayu MSYI, Ullah MS, Takano Y, and Gotoh T

Subjects

Animals, Female, Population Dynamics, Reproduction, Life Cycle Stages physiology, Oviposition physiology, Temperature, Tetranychidae physiology

Abstract

The impact of daily temperature fluctuations on arthropod life history parameters is inadequately studied compared with the ample amount of research that has been conducted on the effects of constant temperatures. Fluctuating temperatures are likely to be more realistic, as they are ecologically more similar to what these arthropods experience in nature. Here, we compared the impact of 11 constant temperatures that ranged from 10 to 35 °C with fluctuating temperatures with the same corresponding mean temperature and an amplitude of 10 °C between high (12 h) and low (12 h) temperatures on the development and life history parameters of Tetranychus urticae under continuous light conditions. No eggs hatched at constant 10 °C, whereas 81.5% of eggs successfully completed development at fluctuating 10 °C (15/5 °C). Egg-to-female adult development was faster under fluctuating temperatures from 12.5 to 27.5 °C than under constant temperatures, whereas the opposite trend was observed at >30 °C. The lower thermal thresholds (T) were 11.63 and 8.63 °C, and thermal constants (K) were 127.81 and 150.69 degree-days for egg-to-female adults at constant and fluctuating temperatures, respectively. The numbers of oviposition days were significantly higher at fluctuating 15 °C than at the corresponding constant temperature, whereas the opposite trend was observed from 20 to 30 °C. The intrinsic rate of increase (r) was higher at fluctuating than at constant 15 °C. The net reproductive rate (R 0 ) was also higher at fluctuating than at constant 15 and 35 °C, but showed an opposite trend at 20 and 25 °C. We conclude that fluctuating temperatures should be considered to accurately predict spider mite population dynamics in nature.

Published

2017

248. Estimating the development rate of the tomato leaf miner, Tuta absoluta (Lepidoptera: Gelechiidae), using linear and non-linear models.

Author

Marchioro CA, Krechemer FS, and Foerster LA

Subjects

Animals, Life Cycle Stages physiology, Solanum lycopersicum parasitology, Moths embryology, Moths physiology, Linear Models, Moths growth & development, Nonlinear Dynamics, Temperature

Abstract

Background: Tuta absoluta Meyrick (Lepidoptera: Gelechiidae) is native to South America and has recently invaded European, African and Asian countries, where it is causing severe damage to tomato crops leading to an increase in the number of insecticide applications. This situation has prompted a demand for alternative pest management strategies aiming to control T. absoluta and concomitantly reduce insecticide applications. The development period for immature stages of T. absoluta at constant temperatures was modelled to select appropriate mathematical functions for simulating its development., Results: The performance of the models varied according to the insect development stage, but in general all models performed well considering the statistical criteria used. Discrimination among models was possible only when the reliability of the temperature thresholds estimated by the models was used as an additional criterion. In this case, the models Briere-1, Lactin-2 and Shi proved adequate to describe the relationship between temperature and development rate of T. absoluta., Conclusion: These models provide an important tool to predict the occurrence of the immature stages of T. absoluta in the field in order to determine the best period for implementing control measures. This is an important contribution to the development of pest management strategies for T. absoluta. © 2016 Society of Chemical Industry., (© 2016 Society of Chemical Industry.)

Published

2017

249. The Life Cycle of Didymium laxifilum and Physarum album on Oat Agar Culture.

Author

Gao Y, Tao W, Yan SZ, and Chen SL

Subjects

Axenic Culture, Microscopy, Electron, Scanning, Morphogenesis, Myxomycetes classification, Physarum classification, Spores, Protozoan growth & development, Wood parasitology, Life Cycle Stages physiology, Myxomycetes growth & development, Physarum growth & development

Abstract

The plasmodial slime molds is the largest group in the phylum Amoebozoa. Its life cycle includes the plasmodial trophic stage and the spore-bearing fruiting bodies. However, only a few species have their complete life cycle known in details so far. This study is the first reporting the morphogenesis of Didymium laxifilum and Physarum album. Spores, from field-collected sporangia, were incubated into hanging drop cultures for viewing germination and axenic oat agar plates for viewing plasmodial development and sporulation. The spores of D. laxifilum and P. album germinated by method of V-shape split and minute pore, respectively. The amoeboflagellates, released from spores, were observed in water film. The phaneroplasmodia of two species developed into a number of sporangia by subhypothallic type on oat agar culture. The main interspecific difference of morphogenesis was also discussed., (© 2016 The Author(s) Journal of Eukaryotic Microbiology © 2016 International Society of Protistologists.)

Published

2017

250. Peptides Selected Using Phage Library Variants, Effectively Inhibit Trypanosoma cruzi Infection.

Author

Kleshchenko YE, Zhigunova AV, Dalin MV, and Melnikov V

Subjects

Amino Acid Sequence, Binding Sites, Biotinylation, HeLa Cells, Humans, Life Cycle Stages physiology, Oligopeptides metabolism, Protein Binding, Trypanocidal Agents metabolism, Trypanosoma cruzi growth & development, Trypanosoma cruzi metabolism, Life Cycle Stages drug effects, Oligopeptides pharmacology, Peptide Library, Trypanocidal Agents pharmacology, Trypanosoma cruzi drug effects

Abstract

Four peptide sequences characterized by high content of hydrophobic, charged, and polar amino acids were obtained from 23 clones of M13 phage. Peptides P2 and P4 exhibited highest binding affinity for immobilized trypomastigotes. The inhibitory effects of peptides seemed to be due to blockade of certain epitopes on T. cruzi surface proteins responsible for interactions with the respective receptors of host cells.

Published

2017