Aug
12
Mon
2013
Invited Talk: Control of sequential movements: insights from the oculomotor system @ Amriteshwari Hall
Aug 12 @ 2:26 pm – 2:54 pm

adityaAditya Murthy, Ph.D.
Associate Professor, Centre For Neuroscience, Indian Institute of Science, Bangalore, India


Since Karl Lashley’s seminal work on the formulation of serial order, numerous models assume simultaneous representation of competitive elements of a sequence, to account for serial order effects in different types of behavior like typing, speech, etc. Such models follow two basic assumptions: (1) more than one plan representation can be simultaneously active in a planning layer; (2) the most active plan is chosen in another layer called the competitive choice layer. Using the oculomotor system I will describe behavioral and neurophysiological experiments that tests the two critical predictions of such queuing models, providing evidence that basal ganglia in monkeys and humans instantiate a form of queuing that transforms parallel movement representations into more serial representations, allowing for the expression of sequential saccadic eye movements.

Aditya Murthy (2)

Aug
13
Tue
2013
Invited Talk: Interrogating Signaling Networks at the Single Cell Level in Primary Human Patient Samples @ Acharya Hall
Aug 13 @ 10:52 am – 11:22 am

MIchelleMichelle Hermiston, MD, Ph.D.
Assistant Professor, Department of Pediatrics University of California San Francisco, USA


Interrogating Signaling Networks at the Single Cell Level In Primary Human Patient Samples

Multiparameter phosphoflow cytometry is a highly sensitive proteomic approach that enables monitoring of biochemical perturbations at the single cell level. By combining antisera to cell surface markers and key intracellular proteins, perturbations in signaling networks, cell survival and apoptosis mediators, cell cycle regulators, and/or modulators of other cellular processes can be analyzed in a highly reproducible and sensitive manner in the basal state and in response to stimulation or drug treatment. Advantages of this approach include the ability to identify the biochemical consequences of genetic and/or epigenetic changes in small numbers of cells, to map potential interplay between various signaling networks simultaneously in a single cell, and to interrogate potential mechanisms of drug resistance or response in a primary patient sample. Application of this technology to patients with acute lymphoblastic leukemia or the autoimmune disease systemic lupus erythematosus (SLE) will be discussed.