Your search keyword '"Aram, D."' showing total 8 results

1. Molecular evolution of the moonlighting protein SMN in metazoans

Author

Shaun Gu, Marsha Dillon-White, and Aram D. Stump

Subjects

Protein moonlighting, Physiology, Biology, Biochemistry, Evolution, Molecular, Negative selection, Molecular evolution, Genetics, Animals, snRNP, Amino Acid Sequence, Molecular Biology, Gene, Conserved Sequence, Phylogeny, Binding Sites, Models, Genetic, Computational Biology, Bayes Theorem, SMN Complex Proteins, Survival of motor neuron, Survival of Motor Neuron 1 Protein, nervous system diseases, nervous system, Small nuclear ribonucleoprotein, Function (biology)

Abstract

The spinal muscular atrophy (SMA) associated protein survival of motor neuron (SMN) is known to be a moonlighting protein: having one primary, ancestral function (presumed to be involvement in U snRNP assembly) along with one or more secondary functions. One hypothesis for the evolution of moonlighting proteins is that regions of a structure under relatively weak negative selection could gain new functions without interfering with the primary function. To test this hypothesis, we investigated sequence conservation and dN/dS, which reflects the selection acting on a coding sequence, in SMN and a related protein, splicing factor 30 (SPF30), which is not currently known to be multifunctional. We found very different patterns of evolution in the two genes, with SPF30 characterized by strong sequence conservation and negative selection in most animal taxa investigated, and SMN with much lower sequence conservation, and much weaker negative selection at many sites. Evidence was found of positive selection acting on some sites in primate genes for SMN. SMN was also found to have been duplicated in a number of species, and with patterns that indicate reduced negative selection following some of these duplications. There were also several animal species lacking an SMN gene.

Published

2013

2. Selective constraint and the evolution of the RNA Polymerase II C-Terminal Domain

Author

Aram D. Stump and Khrystyna Ostrozhynska

Subjects

Repetitive Sequences, Amino Acid, Protein subunit, RNA polymerase II, Biology, Biochemistry, Evolution, Molecular, Negative selection, Transcription (biology), Phylogenetics, Genetics, dN/dS, Animals, Phylogeny, Leishmania, C-terminus, Fungi, Plants, biology.organism_classification, CTD, Protein Structure, Tertiary, biology.protein, selective constraint, Eukaryote, RNA Polymerase II, purifying selection, eukaryote evolution, Biotechnology, Research Paper

Abstract

The C-Terminal Domain (CTD) of the large subunit (Rpb1) of RNA Polymerase II has a Tyrosine-Serine-Proline-Threonine-Serine-Proline-Serine repeat structure in many eukaryotes. Chemical modifications of these residues play a central role in the regulation and coordination of the events of transcription. However, substantial variability in the presence and regularity of repeat arrays exists between eukaryote taxa. Following a survey of CTD structure from diverse eukaryote species, two hypotheses were tested relating to repeat structure and the action of selection on the CTD. First, it was found that degenerated repeat structure is associated with lower serine and proline frequencies in some eukaryote taxa but not in others. Second, maximum likelihood models of the evolution of Rpb1 in a number of species groups found that purifying selection on the non-repetitive CTD of several Leishmania species was substantially lower than for the rest of Rpb1, whereas purifying selection in a number of species groups containing repeat arrays was usually as high or nearly as high as for the rest of Rpb1. Characterization of CTD structure for a larger number of species than has been completed previously also revealed a greater diversity of CTD structures in eukaryotes than previously known, along with loss of repeat structure in the animals and fungi, two taxa where it has not previously been known. These results suggest that loss of CTD repeat structure has been an important aspect of RNA Polymerase II evolution in diverse eukaryotes.

Published

2013

3. Distribution and Mechanism of α-Amanitin Tolerance in Mycophagous Drosophila (Diptera: Drosophilidae)

Author

Sara E. Jablonski, Jason A. Wilder, Aram D. Stump, and Lindsay Legault Bouton

Subjects

endocrine system, animal structures, Cytochrome, Piperonyl Butoxide, Amanita, Molecular Sequence Data, Biology, medicine.disease_cause, Models, Biological, Fungal Proteins, Food Preferences, Oregon, Species Specificity, Drosophilidae, Botany, polycyclic compounds, medicine, Animals, Gene, Drosophila, Phylogeny, Ecology, Evolution, Behavior and Systematics, Alpha-Amanitin, Amanitin, chemistry.chemical_classification, Dose-Response Relationship, Drug, Ecology, Toxin, fungi, Cytochrome P450, Sequence Analysis, DNA, Mycotoxins, biology.organism_classification, Ethacrynic Acid, Enzyme, Massachusetts, chemistry, Biochemistry, Larva, Insect Science, Linear Models, biology.protein, Female, RNA Polymerase II, Sequence Alignment

Abstract

Many mycophagous species of Drosophila can tolerate the mushroom poison α-amanitin in wild mushrooms and in artificial diet. We conducted feeding assays with sixteen Drosophila species and α-amanitin in artificial diet to better determine the phylogenetic distribution of this tolerance. For eight tolerant and one related susceptible species, we sequenced the gene encoding the large subunit of RNA Polymerase II, which is the target site of α-amanitin. We found no differences in the gene that could account for differences in susceptibility to the toxin. We also conducted feeding assays in which α-amanitin was combined with chemical inhibitors of cytochrome P450s or glutathione S-transferases (GSTs) in artificial diet to determine if either of these enzyme families is involved in tolerance to α-amanitin. We found that an inhibitor of GSTs did not reduce tolerance to α-amanitin, but that an inhibitor of cytochrome P450s reduced tolerance in several species. It is possible that the same cytochrome P450 activity that produces tolerance of α-amanitin might produce tolerance of other mushroom toxins as well. If so, a general detoxification mechanism based on cytochrome P450s might answer the question of how tolerance to α-amanitin arose in mycophagous Drosophila when this toxin is found in relatively few mushrooms.

Published

2011

4. Genetic exchange in 2La inversion heterokaryotypes of Anopheles gambiae

Author

Alessandra della Torre, José M. C. Ribeiro, N. J. Besansky, Aram D. Stump, J. A. Wilder, L. Goeddel, and Marco Pombi

Subjects

Genetics, Natural selection, biology, Anopheles gambiae, Chromosome, biology.organism_classification, Centimorgan, Insect Science, Backcrossing, Molecular Biology, Genetic isolate, Recombination, Chromosomal inversion

Abstract

In the malaria vector Anopheles gambiae, alternative arrangements of chromosome 2 (2La and 2L+(a)) vary in relative frequency along clines of aridity, suggesting the action of natural selection on targets within the inversion. Our long term goal of detecting such targets depends in part on the level of genetic exchange between arrangements. Accordingly, we estimated recombination rates on 2L from the backcross progeny of 2La/+(a) heterokaryotypes and as a control, from 2L+(a) homokaryotypes. In homokaryotypes, the recombination rate was uniform at ~2.0 centimorgans per megabase (cM/Mb). In heterokaryotypes, recombination within the rearranged region was reduced to < 0.5 cM/Mb, with slightly higher but nevertheless reduced levels (< 1.0 cM/Mb) flanking the rearrangement. Yet, gene exchange was recorded between nearly all markers, including those very near the distal inversion breakpoint. These results suggest that reduced recombination is a necessary but not sufficient mechanism for genetic isolation between alternative arrangements, and that the targets of natural selection can be identified against the different chromosomal backgrounds.

Published

2007

5. Sex-Linked Differentiation Between Incipient Species of Anopheles gambiae

Author

Nora J. Besansky, Aram D. Stump, Jennifer A. Shoener, N’Fale Sagnon, and Carlo Costantini

Subjects

Genetic Markers, Male, Sex Differentiation, X Chromosome, Anopheles gambiae, Locus (genetics), Investigations, DNA, Ribosomal, Linkage Disequilibrium, Species Specificity, Anopheles, parasitic diseases, Centromere, Genetics, Animals, Phylogeny, X chromosome, biology, Chromosome Mapping, DNA, Reproductive isolation, Incipient speciation, biology.organism_classification, Microsatellite, Female, Sex linkage

Abstract

Emerging species within the primary malaria vector Anopheles gambiae show different ecological preferences and significant prezygotic reproductive isolation. They are defined by fixed sequence differences in X-linked rDNA, but most previous studies have failed to detect large and significant differentiation between these taxa elsewhere in the genome, except at two other loci on the X chromosome near the rDNA locus. Hypothesizing that this pericentromeric region of the X chromosome may be accumulating differences faster than other regions of the genome, we explored the pattern and extent of differentiation between A. gambiae incipient species and a sibling species, A. arabiensis, from Burkina Faso, West Africa, at 17 microsatellite loci spanning the X chromosome. Interspecific differentiation was large and significant across the entire X chromosome. Among A. gambiae incipient species, we found some of the highest levels of differentiation recorded in a large region including eight independent loci near the centromere of the X chromosome. Outside of this region, no significant differentiation was detected. This pattern suggests that selection is playing a role in the emergence of A. gambiae incipient species. This process, associated with efficient exploitation of anthropogenic modifications to the environment, has public health implications as it fosters the spread of malaria transmission both spatially and temporally.

Published

2005

6. VARIATION IN RECOMBINATION RATE ACROSS THE X CHROMOSOME OF ANOPHELES GAMBIAE

Author

Nora J. Besansky, Aram D. Stump, Alessandra della Torre, and Marco Pombi

Subjects

Genetics, biology, Anopheles gambiae, Chromosome, Incipient speciation, biology.organism_classification, Centimorgan, Infectious Diseases, Virology, Centromere, Microsatellite, Parasitology, X chromosome, Recombination

Abstract

The M and S molecular forms of Anopheles gambiae are considered to be incipient species, despite residual gene exchange. Of the three small genome regions that are strongly differentiated between the molecular forms ("speciation islands"), two are located near centromeres, on the left arm of chromosome 2 and the X chromosome. To test the prediction of reduced recombination in these islands, we estimated recombination rates between microsatellite loci on the X chromosome using two M-form strains. Across most of the chromosome, recombination occurred at approximately 1 centimorgan per megabase (cM Mb(-1)), a value closely matching the genome-wide average estimated for A. gambiae and for other eukaryotes. Recombination was much higher at the telomeric end, > 7 cM Mb(-1). In the speciation island at the centromeric end, recombination was sharply reduced to approximately 0.2 cM Mb(-1), consistent with a role for reduced recombination in maintaining differentiation between nascent species despite gene flow.

Published

2006

7. Centromere-proximal differentiation and speciation in Anopheles gambiae

Author

Carlo Costantini, Neil F. Lobo, Meagan C. Fitzpatrick, Frank H. Collins, Sekou F. Traore, N’Fale Sagnon, Aram D. Stump, and Nora J. Besansky

Subjects

X Chromosome, Anopheles gambiae, Climate, Centromere, Molecular Sequence Data, Biology, Genetic recombination, Nucleotide diversity, Gene flow, Anopheles, Animals, X chromosome, Phylogeny, Genetics, Recombination, Genetic, Multidisciplinary, Natural selection, Polymorphism, Genetic, Base Sequence, Genetic Drift, Chromosome Mapping, Sequence Analysis, DNA, Biological Sciences, biology.organism_classification, Adaptation, Physiological, Sympatric speciation, Africa, Mutation

Abstract

The M and S molecular forms of Anopheles gambiae are undergoing speciation as they adapt to heterogeneities in the environment, spreading malaria in the process. We hypothesized that their divergence despite gene flow is facilitated by reduced recombination at the centromeric (proximal) end of the X chromosome. We sequenced introns from 22 X chromosome genes in M and S from two locations of West Africa where the forms are sympatric. Generally, in both forms nucleotide diversity was high distally, lower proximally, and very low nearest the centromere. Conversely, differentiation between the forms was virtually zero distally and very high proximally. Pairwise comparisons to a close relative, the sibling species Anopheles arabiensis , demonstrated uniformly high divergence regardless of position along the X chromosome, suggesting that this pattern is not purely mechanical. Instead, the pattern observed for M and S suggests the action of divergent natural selection countering gene flow only at the proximal end of the X chromosome, where recombination is reduced. Comparison of sites with fixed differences between M and S to the corresponding sites in A. arabiensis revealed that derived substitutions had been fixed in both forms, further supporting the hypothesis that both have been under selection. These derived substitutions are fixed in the two West African samples and in samples of S from western and coastal Kenya, suggesting that selection occurred before the forms expanded to their current ranges. Our findings are consistent with a role for suppressed genetic recombination in speciation of A. gambiae .

Published

2005

8. Genetic structure of Anopheles gambiae populations on islands in northwestern Lake Victoria, Uganda

Author

Frank H. Collins, Louis G. Mukwaya, Aram D. Stump, Andrew P. Michel, Mamadou B. Coulibaly, Nora J. Besansky, and Jonathan K. Kayondo

Subjects

Gene Flow, lcsh:Arctic medicine. Tropical medicine, Time Factors, Genotype, lcsh:RC955-962, Anopheles gambiae, 030231 tropical medicine, Polymerase Chain Reaction, lcsh:Infectious and parasitic diseases, Gene flow, 03 medical and health sciences, 0302 clinical medicine, Effective population size, Genetic variation, Anopheles, Animals, lcsh:RC109-216, Uganda, 030304 developmental biology, Population Density, 0303 health sciences, Polymorphism, Genetic, biology, Geography, Ecology, Research, Genetic Variation, Small population size, biology.organism_classification, 3. Good health, Insect Vectors, Infectious Diseases, Vector (epidemiology), Genetic structure, Chromosome Inversion, Linear Models, Parasitology, Mainland, Microsatellite Repeats

Abstract

Background Alternative means of malaria control are urgently needed. Evaluating the effectiveness of measures that involve genetic manipulation of vector populations will be facilitated by identifying small, genetically isolated vector populations. The study was designed to use variation in microsatellite markers to look at genetic structure across four Lake Victoria islands and two surrounding mainland populations and for evidence of any restriction to free gene flow. Methods Four Islands (from 20–50 km apart) and two surrounding mainland populations (96 km apart) were studied. Samples of indoor resting adult mosquitoes, collected over two consecutive years, were genotyped at microsatellite loci distributed broadly throughout the genome and analysed for genetic structure, effective migration (Nem) and effective population size (Ne). Results Ne estimates showed island populations to consist of smaller demes compared to the mainland ones. Most populations were significantly differentiated geographically, and from one year to the other. Average geographic pair-wise F ST ranged from 0.014–0.105 and several pairs of populations had Ne m < 3. The loci showed broad heterogeneity at capturing or estimating population differences. Conclusion These island populations are significantly genetically differentiated. Differences reoccurred over the study period, between the two mainland populations and between each other. This appears to be the product of their separation by water, dynamics of small populations and local adaptation. With further characterisation these islands could become possible sites for applying measures evaluating effectiveness of control by genetic manipulation.

Published

2005