Cherian Zachariah
University of Florida
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Publication
Featured researches published by Cherian Zachariah.
Nature | 2008
Jagan Srinivasan; Fatma Kaplan; Ramadan Ajredini; Cherian Zachariah; Hans T. Alborn; Peter E. A. Teal; Rabia U. Malik; Arthur S. Edison; Paul W. Sternberg; Frank C. Schroeder
In many organisms, population-density sensing and sexual attraction rely on small-molecule-based signalling systems. In the nematode Caenorhabditis elegans, population density is monitored through specific glycosides of the dideoxysugar ascarylose (the ‘ascarosides’) that promote entry into an alternative larval stage, the non-feeding and highly persistent dauer stage. In addition, adult C. elegans males are attracted to hermaphrodites by a previously unidentified small-molecule signal. Here we show, by means of combinatorial activity-guided fractionation of the C. elegans metabolome, that the mating signal consists of a synergistic blend of three dauer-inducing ascarosides, which we call ascr#2, ascr#3 and ascr#4. This blend of ascarosides acts as a potent male attractant at very low concentrations, whereas at the higher concentrations required for dauer formation the compounds no longer attract males and instead deter hermaphrodites. The ascarosides ascr#2 and ascr#3 carry different, but overlapping, information, as ascr#3 is more potent as a male attractant than ascr#2, whereas ascr#2 is slightly more potent than ascr#3 in promoting dauer formation. We demonstrate that ascr#2, ascr#3 and ascr#4 are strongly synergistic, and that two types of neuron, the amphid single-ciliated sensory neuron type K (ASK) and the male-specific cephalic companion neuron (CEM), are required for male attraction by ascr#3. On the basis of these results, male attraction and dauer formation in C. elegans appear as alternative behavioural responses to a common set of signalling molecules. The ascaroside signalling system thus connects reproductive and developmental pathways and represents a unique example of structure- and concentration-dependent differential activity of signalling molecules.
Journal of Chemical Ecology | 2009
Fatma Kaplan; Dayakar V. Badri; Cherian Zachariah; Ramadan Ajredini; Francisco J. Sandoval; Sanja Roje; Lanfang H. Levine; Fengli Zhang; Steven L. Robinette; Hans T. Alborn; Wei Zhao; Michael Stadler; Rathika Nimalendran; Aaron T. Dossey; Rafael Brüschweiler; Jorge M. Vivanco; Arthur S. Edison
Caenorhabditis elegans, a bacterivorous nematode, lives in complex rotting fruit, soil, and compost environments, and chemical interactions are required for mating, monitoring population density, recognition of food, avoidance of pathogenic microbes, and other essential ecological functions. Despite being one of the best-studied model organisms in biology, relatively little is known about the signals that C. elegans uses to interact chemically with its environment or as defense. C. elegans exudates were analyzed by using several analytical methods and found to contain 36 common metabolites that include organic acids, amino acids, and sugars, all in relatively high abundance. Furthermore, the concentrations of amino acids in the exudates were dependent on developmental stage. The C. elegans exudates were tested for bacterial chemotaxis using Pseudomonas putida (KT2440), a plant growth promoting rhizobacterium, Pseudomonas aeruginosa (PAO1), a soil bacterium pathogenic to C. elegans, and Escherichia coli (OP50), a non-motile bacterium tested as a control. The C. elegans exudates attracted the two Pseudomonas species, but had no detectable antibacterial activity against P. aeruginosa. To our surprise, the exudates of young adult and adult life stages of C. elegans exudates inhibited quorum sensing in the reporter system based on the LuxR bacterial quorum sensing (QS) system, which regulates bacterial virulence and other factors in Vibrio fischeri. We were able to fractionate the QS inhibition and bacterial chemotaxis activities, thus demonstrating that these activities are chemically distinct. Our results demonstrate that C. elegans can attract its bacterial food and has the potential of partially regulating the virulence of bacterial pathogens by inhibiting specific QS systems.
Current protocols in protein science | 2007
Mini Samuel‐Landtiser; Cherian Zachariah; Christopher R. Williams; Arthur S. Edison; Joanna R. Long
The incorporation of isotope labels into proteins is extremely useful for the application of nuclear magnetic resonance (NMR), X‐ray or neutron‐diffraction crystallography, and mass spectrometry (MS) methodologies to investigate the structure and dynamics of proteins. This unit presents methods for incorporating isotopic labels into proteins via expression in E. coli and baculovirus transfected Sf9 insect cells or through cell‐free means. The unit also presents methods for introducing isotopic labels by chemical means into synthetic peptides by solid phase peptide synthesis or into isolated proteins by chemical modification of labile protein groups.
Analytical Chemistry | 2007
Fengli Zhang; Aaron T. Dossey; Cherian Zachariah; Arthur S. Edison; Rafael Brüschweiler
Physical Review Letters | 2003
Linlin Qiu; Cherian Zachariah; Stephen J. Hagen
Biochemistry | 2003
Leif Smith; Cherian Zachariah; Ramanan Thirumoorthy; Jim Rocca; Jan Novak; J. D. Hillman; Arthur S. Edison
Magnetic Resonance in Chemistry | 2006
Yu Li; Andrew G. Webb; Saikat Saha; William W. Brey; Cherian Zachariah; Arthur S. Edison
The Journal of Neuroscience | 1999
Arthur S. Edison; Eduardo Espinoza; Cherian Zachariah
Biochemistry | 2006
Aaron T. Dossey; Heather Chatwin; Cherian Zachariah; Mario deBono; Peter D. Evans; Arthur S. Edison
Biochemistry | 2001
Cherian Zachariah; Angus Cameron; Iris Lindberg; K. J. Kao; Margery C. Beinfeld; Arthur S. Edison