http://www.nature.com/news/big-biology-the-omes-puzzle-1.12484?WT.ec_id=NATURE-20130228
‘Omics discussion in Nature


SYLICA Synthetic Biology – Bowater Feb 2013
SYLICA 2013
Bowater lectures
Synthetic Biology & Nanotechnology: Tomorrow’s Molecular Biology?

Bowater Lectures in Brno, Feb. 2013
4 lectures on linked topics will be delivered during the coming week:
•Contemporary DNA Sequencing Technologies – 26/2/2013 @ 10:00
•Using ‘Omic Technologies to Investigate Gene Function – 26/2/2013 @ 14:00
•Biophysical Methods to Study Molecular Interactions – 27/2/2013 @ 10:00
•Synthetic Biology & Nanotechnology: Tomorrow’s Molecular Biology? – 28/2/2013 @ 10:00
SYLICA Synthetic Biology – Bowater Feb 2013

Nanotechnology & Synthetic Biology
•Presentation will discuss two overlapping topics:
ØNanotechnology
ØSynthetic Biology (incorporating metabolic engineering and protein engineering)
•These are emerging disciplines, covering vast areas of science – not just biology!
•Here it is only possible to introduce the topics and provide some brief discussion of specific
examples
SYLICA Synthetic Biology – Bowater Feb 2013
•To ensure that we are all clear where the discussion should start, it is useful to include some
definitions….

Nanotechnology
•Nanotechnology….
ØLiterally defined as: Technology that is useful on the nanoscale – 1-100 nm (atom scale = 0.1 nm)
ØFor biologists, this is more usefully defined as: manipulation of biological molecules/structures
to produce useful materials or devices
•Biological molecules used in such technology must be stable for their required use e.g. uses of
proteins will provide different opportunities to nucleic acids
•Requires collaboration of molecular biologists with experts in quantum physics, organic chemistry,
surface science, computer science….etc.
SYLICA Synthetic Biology – Bowater Feb 2013

The combination of engineering with biology to engineer living things to create novel:
Fuels, Medicines , and Materials
The overall aims are to solve the Grand Challenges of the 21st Century
Synthetic Biology
SYLICA Synthetic Biology – Bowater Feb 2013
[USEMAP]
Explanation on Youtube: http://www.youtube.com/watch?v=rD5uNAMbDaQ

DNA Nanotechnology
•DNA is appropriate for nanotechnological methods for several reasons:
ØIt is a (relatively) stable chemical, which exists in different forms (nucleotides, nucleic acids)
ØAs a polymer it can form very long molecules
ØIt has a well defined, repetitive structure
Ø“Rules” for determining the structure are simple and well-understood
ØWithin the molecule many atoms are available to form useful interactions/modifications
SYLICA Synthetic Biology – Bowater Feb 2013

DNA Origami
•During the 1980’s, studies of DNA highlighted that complex structures could be formed
•Since these structures are stabilised by base pairs in the molecule, it became clear that the
complex structures could be created using carefully-designed DNA sequences
•Importantly, the complex structures can be built up from simpler molecules
Ø
SYLICA Synthetic Biology – Bowater Feb 2013

DNA Origami
SYLICA Synthetic Biology – Bowater Feb 2013
Seeman, 2010, Ann. Rev. Biochem., 79, 65-87

DNA Origami
SYLICA Synthetic Biology – Bowater Feb 2013
Seeman, 2010, Ann. Rev. Biochem., 79, 65-87
Seeman Fig 4.jpg

DNA Origami
SYLICA Synthetic Biology – Bowater Feb 2013
Seeman, 2010, Ann. Rev. Biochem., 79, 65-87

DNA Origami: Examples
SYLICA Synthetic Biology – Bowater Feb 2013
Pinheiro et al., 2011, Nat. Nanotech., 6, 763-772

Applications of DNA Nanotechnology
•Not just for creating beautiful pictures….
SYLICA Synthetic Biology – Bowater Feb 2013
Pinheiro et al., 2011, Nat. Nanotech., 6, 763-772
figure 6.jpg

Synthetic Biology
SYLICA Synthetic Biology – Bowater Feb 2013


Synthia: a Synthetic Bacterium
SYLICA Synthetic Biology – Bowater Feb 2013
Gibson et al., 2010, Science, 329, 52-56
•This paper reported the design, synthesis, and assembly of the 1.08–mega–base pair Mycoplasma
mycoides JCVI-syn1.0 genome
•The genome was chemically synthesised and transplanted into a M. capricolum recipient cell
•The new M. mycoides cells are controlled by the synthetic chromosome, which also includes
“watermark” sequences, designed gene deletions and polymorphisms, and mutations acquired during the
building process
•The new cells have expected phenotypic properties and are capable of continuous self-replication

Expression Systems
•Most widely used system to express recombinant proteins is E. coli
•Need:
-Expression vector (plasmid)
-Specific bacterial strains
•Many specialised expression systems and strains have been developed
•
SYLICA Synthetic Biology – Bowater Feb 2013

Bacterial Expression Strains
•Number of different bacterial strains are in use
•One of most widely used is E. coli BL21
•Takes advantage of a viral RNA polymerase, so will only express genes prepared downstream of viral
promoter
Novagen pET system manual, 11th ed
•Strains altered to allow different types of control of gene expression
•Strains also produced that allow expression of different types of genes
SYLICA Synthetic Biology – Bowater Feb 2013

Codon Bias
•Different organisms have differences in their usage of (A+T) and (G+C)
•Leads to different biases in their use of codons and anti-codons
•Strains of E. coli BL21 have been developed that can make tRNAs to allow them to cope with
variation in codon usage e.g. Origami, Rosetta, etc.
Escherichia coli
http://www.kazusa.or.jp/java/codon_table_java/
http://www.kazusa.or.jp/java/codon_table_java/
Humans
SYLICA Synthetic Biology – Bowater Feb 2013

Other Expression Strains
•E. coli expression systems are very powerful but sometimes have problems
•A better approach can be to try to express protein in native cell (or something similar)
-Different types of bacteria
-Yeast are widely used e.g. Pichia pastoris
-Insect cells in culture
-Mammalian cells in culture
SYLICA Synthetic Biology – Bowater Feb 2013

Metabolic Engineering
•Metabolic Engineering – or “Biotransformations” – relates to use of biological catalysts to
produce specific, desired products
•Usually enzymes, but can be whole organisms
•Industry uses this to produce food, pharmaceuticals, detergents, agricultural chemicals, etc.
•
SYLICA Synthetic Biology – Bowater Feb 2013

Process Development
Genetic engineering
Protein engineering
Product concentration
Volumetric productivity
•Quality
•Purity
•Scale
Substrates
Screening & selection of biocatalysts
Biocatalyst production (fermentation/purification)
Medium engineering
Design & scale-up of bio-reactor
Product isolation & purification
Product
Basic Biotechnology, 2006, Ratledge & Kristiansen, 3rd edn, Fig. 24.1
SYLICA Synthetic Biology – Bowater Feb 2013

Metabolic Engineering - Advantages
•Use of enzymes/organisms has number of possible advantages compared to what can be achieved by
chemical industry:
-Simpler
-Less raw materials and energy
-Higher quality products
-Higher yields
-Decrease toxic wastes and wastewater
-Lower costs and environmentally friendly??
SYLICA Synthetic Biology – Bowater Feb 2013

Compounds Produced by Commercial-scale Bioprocesses
•Alcohols
•Amino acids
•Antibiotics
•Polymers
-Starch
-Polyurethane
•Sweeteners
•Vitamins
•
SYLICA Synthetic Biology – Bowater Feb 2013

Prokaryotes used in Biotransformations
•Wide range of prokaryotes used in biotransformations, including:
ØEscherichia coli: Gamma-proteobacteria; widely used in development processes, produce amino acids
ØMycobacterium spp: Actinobacteria; various agricultural and medical compounds
ØRhodococcus rhodochrous: produces acrylamide
ØStreptomyces coelicolor: Actinobacteria; antibiotics + wide range of other metabolites
SYLICA Synthetic Biology – Bowater Feb 2013

•A number of diverse bacteria used as models for metabolic engineering
•Microbial genome sequences have revealed many examples of ‘cryptic’ or ‘orphan’ biosynthetic gene
clusters
•Have potential to direct the production of novel, structurally complex natural products
•Synthetic biology will provide new mechanisms, roles and specificities for natural product
biosynthetic enzymes
SYLICA Synthetic Biology – Bowater Feb 2013
Prokaryotes used in Biotransformations

Tagged Proteins
•“Tags” are widely used to give convenient, fast purification of recombinant proteins (via affinity
chromatography)
•One “tag” is Glutathione-S-transferase (GST)
•GST is a small enzyme that binds glutathione (Glu to which Cys-Gly is attached)
•GST tags are usually placed at C-terminus of proteins
SYLICA Synthetic Biology – Bowater Feb 2013

Different Types of Tags
SYLICA Synthetic Biology – Bowater Feb 2013


Fluorescently-tagged Proteins
•Combination of molecular and cell biological studies analyse in vivo localisation of proteins
expressed with a fluorescent “tag”
•Important that “tag” does not interfere with protein activity
•
•
•
•
Bastiaens & Pepperkok (2000) TiBS, 25, 631-637
•Can examine localisation of proteins containing different fluorophores
SYLICA Synthetic Biology – Bowater Feb 2013

GFP–Tagged Protein Localization
SYLICA Synthetic Biology – Bowater Feb 2013

FIGURE 9–16 Green fluorescent protein (GFP). (a) The GFP protein (PDB ID 1GFL), derived from the
jellyfish Aequorea victoria, has a β-barrel structure; the fluorophore (shown as a space-filling
model) is in the center of the barrel. (b) Variants of GFP are now available in almost any color of
the visible spectrum. (c) A GLR1-GFP fusion protein fluoresces bright green in Caenorhabditis
elegans, a nematode worm (left). GLR1 is a glutamate receptor of nervous tissue. (Autofluorescing
fat droplets are false colored in magenta.) The membranes of E. coli cells (right) are stained with
a red fluorescent dye. The cells are expressing a protein that binds to a resident plasmid, fused
to GFP. The green spots indicate the locations of plasmids.

Biotechnological Applications
•Protein engineering approaches can be used to provide significant alterations to cell function
•Such changes bring forward important ethical and moral issues that need to be addressed
SYLICA Synthetic Biology – Bowater Feb 2013

Medical Applications
•Protein engineering is also finding increasing uses in human medicine
•Again, such uses have important ethical and moral issues that need to be addressed
SYLICA Synthetic Biology – Bowater Feb 2013

Protein Engineering
•In all cells proteins have:
-Enzyme activities
-Structural roles
•In past 50 years scientists have learned how to prepare large amounts of pure proteins
•Allows detailed in vitro studies
•Proteins can also be made to do useful operations both in vitro and in cells
•Protein engineering involves processes that modify or improve proteins
SYLICA Synthetic Biology – Bowater Feb 2013

Improving Proteins
•Quite difficult to improve on activities of proteins for any particular cell – evolution is very
efficient!
•Can replace mutated (dysfunctional) proteins
•Recent advances have tried to make use of novel or uncommon amino acids
-Selenocysteine: in a few proteins in all cells (e.g. formate dehydrogenase in bacteria,
glutathione peroxidase in mammals)
-Pyrrolysine: found in methanogenic group of Archaea
•
SYLICA Synthetic Biology – Bowater Feb 2013

Uncommon Amino Acids
•Expansion of genetic code to uncommon amino acids requires several changes in cells:
-Specific aminoacyl-tRNA synthetase
-Specific tRNA
-New metabolic pathways (??) for synthesis of above molecules
•
•
•Scientists have used similar approaches to incorporate unnatural amino acids
•Added one at a time, but over 30 different amino acids have been introduced
•Performed for E. coli, yeast, mammalian cells
(a) ketone; (b) azide; (c) photocrosslinker; (d) highly fluorescent; (e) heavy atom for use in
crystallography; (f) long-chain cysteine analogue
SYLICA Synthetic Biology – Bowater Feb 2013

Tomorrow’s Molecular Biology: Overview
•Biology offers a range of molecules that can be manipulated to produce useful materials or devices
•Synthetic biology incorporates “engineering” approaches to take advantage of and improve
biological systems to tackle specific problems
•Protein Engineering manipulates protein production, incorporating modifications to “improve”
proteins
•Recombinant proteins can provide much information about protein function both in vitro and in vivo
•Engineered proteins have huge potentials in biotechnology and medicine
•Important ethical and moral issues to overcome
SYLICA Synthetic Biology – Bowater Feb 2013

A Global Synthetic Biology Competition for Undergraduate Students
iGEM: What is it?
SYLICA Synthetic Biology – Bowater Feb 2013
iGEM: International Genetically Engineered Machines
Organised by the iGEM Foundation, a spin out from the MIT in the USA

SYLICA Synthetic Biology – Bowater Feb 2013
What is Involved in iGEM?
•The team (Students + Advisers) develop a Synthetic Biology Project that must be completed during
the summer months
•Teams compete to win medals (Gold, Silver or Bronze) and prizes
•
•Genetic engineering must be perfromed within the project, following quite strict criteria
•Also must involve Human Practices (outreach) and consideration of ethical issues related to the
project

Find out what we did:
Facebook: www.facebook.com/UEAJIC.IGEM
Twitter: www.twitter.com/UEAJIC_IGEM
Wiki: http://2011.igem.org/Team:UEA-JIC_Norwich
In October 2011 the UEA-JIC_iGEM Team attended the iGEM Jamboree in Amsterdam

NRP-UEA iGEM Team 2012
In 2012 we organised the 2nd iGEM team based on the Norwich Research Park
For info: see http://2012.igem.org/
Team:NRP-UEA-Norwich
Our team included 7 undergraduate students from BIO
We were predominantly based at the School of Biological Sciences at UEA