Hana El-Samad, PhD Grace Boyer Jr. Endowed Chair Biochemistry and Biophysics
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Hana El-Samad, PhD Grace Boyer Jr. Endowed Chair Biochemistry and Biophysics California Institute for Quantitative Biosciences (QB3) University of California, San Francisco Design Principles for Cellular Organization
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Design Principles for Cellular Organization. Hana El-Samad, PhD Grace Boyer Jr. Endowed Chair Biochemistry and Biophysics California Institute for Quantitative Biosciences (QB3) University of California, San Francisco. Some shared principles between the computing and biological sciences. - PowerPoint PPT Presentation
Transcript of Hana El-Samad, PhD Grace Boyer Jr. Endowed Chair Biochemistry and Biophysics
Hana El-Samad, PhDGrace Boyer Jr. Endowed Chair
Biochemistry and BiophysicsCalifornia Institute for Quantitative Biosciences (QB3)University of California, San Francisco
Design Principles for Cellular Organization
Some shared principlesbetween the computing and biological sciences
• Large number of components and complex interactions.
• Extensive use of feedback.
• Versatile modes of control (centralized and distributed).
• “design” for performance and associated tradeoffs.
• Modularity (?).
Some Important future research directions
• Deciphering and defining differences between biology and engineering systems.
• Eliminating “the fold-change” mentality (embrace the subtle, dynamic phenotype).
• Understanding stochasticity (beyond simplistic conclusions).
Conceptual:
Methodological
• Dealing with/modeling uncertainty. • Identifiability. • Measuring/exploiting information about dynamics.• Bridging scales in time and space.
Difference: Crosstalk and Insulation
Deep sub-micron effectsProximity of transistors and leakage of
electrons
Many shared/reused components in natural circuits
Example biological networks that monitor and respond to environment
How do interconnected networks achieve appropriate output to specific inputs?
Annihilation of signaling(degradation)
?
?
One solution: Following the signal
GeneAutomaton: Automation Infrastructure for High-throughput Single Cell Dynamic Measurements
Ignacio Zuleta,, Hao Li
GeneAutomaton is up and running!
Embrace the subtle, dynamic phenotype
The Unfolded Protein Response (UPR)
An intracellular signaling pathway connecting the ER and the nucleus
The cellular response to protein folding stress in the ER
A model for the regulation of organelle abundance
Activated in cancer, protein folding and neurodegenerative disease
The UPR in yeast: Ire1 Signaling Pathway in lead role
1. Unfolded proteins trigger Ire1 oligomerization
2. Oligomerization activates Ire1’s endo-ribonuclease domain in the cytoplasm
3. Active RNase cleaves non-conventional intron from its substrate mRNA, HAC1/XBP1
4. Exons ligated by tRNA ligase, and mature transcript translated to produce a transcriptional activator of UPR target genes
5. Feedback that fixes problem: homeostasis
Doses of DTT that won’t stunt population growth
What regulatory components of UPR modulate dose-to-duration behavior?
Looking at dynamics, and embracing the subtle, a 15-year old enigma is resolved
Pincus et al, PloS Biology, in press
Some mentoring and resoures for the next generation of scientists
• The obvious: more quantitative training for life-scientists.
• Quantitative vs. qualitative understanding (parts list versus system understanding).
• Lower energy barrier for physical-scientists to transition.– Mathematical vs. biological question– A problem of equity: scarce financial resources (fellowships) for re-
training.
