The construction of a minimal cell that exhibits the essential characteristics of life is a great challenge in the field of synthetic biology. Assembling a minimal cell requires multidisciplinary expertise from physics, chemistry and biology. Scientists from different backgrounds tend to define the essence of 'life' differently and have thus proposed different artificial cell models possessing one or several essential features of living cells. Using the tools and methods of molecular biology, the bottom-up engineering of a minimal cell appears in reach. However, several challenges still remain. In particular, the integration of individual sub-systems that is required to achieve a self-reproducing cell model presents a complex optimization challenge. For example, multiple self-organisation and self-assembly processes have to be carefully tuned. We review advances and developments of new methods and techniques, for cell-free protein synthesis as well as micro-fabrication, for their potential to resolve challenges and to accelerate the development of minimal cells.
Reconstituting
functional modules of biological systems in vitro
is an important yet challenging goal of bottom-up synthetic biology,
in particular with respect to their precise spatiotemporal regulation.
One of the most desirable external control parameters for the engineering
of biological systems is visible light, owing to its specificity and
ease of defined application in space and time. Here we engineered
the PhyB-PIF6 system to spatiotemporally target proteins by light
onto model membranes and thus sequentially guide protein pattern formation
and structural assembly in vitro from the bottom up. We show that
complex micrometer-sized protein patterns can be printed on time scales
of seconds, and the pattern density can be precisely controlled by
protein concentration, laser power, and activation time. Moreover,
when printing self-assembling proteins such as the bacterial cytoskeleton
protein FtsZ, the targeted assembly into filaments and large-scale
structures such as artificial rings can be accomplished. Thus, light
mediated sequential protein assembly in cell-free systems represents
a promising approach to hierarchically building up the next level
of complexity toward a minimal cell.
The growth and production of microorganisms in bioconversion are often hampered by heat stress. In this study, an intelligent microbial heat-regulating engine (IMHeRE) was developed and customized to improve the thermo-robustness of Escherichia coli via the integration of a thermotolerant system and a quorum-regulating system. At the cell level, the thermotolerant system composed of different heat shock proteins and RNA thermometers hierarchically expands the optimum temperature by sensing heat changes. At the community level, the quorum-regulating system dynamically programs the altruistic sacrifice of individuals to reduce metabolic heat release by sensing the temperature and cell density. Using this hierarchical, dynamical, and multilevel regulation, the IMHeRE is able to significantly improve cell growth and production. In a real application, the production of lysine was increased 5-fold at 40 °C using the IMHeRE. Our work provides new potential for the development of bioconversion by conserving energy and increasing productivity.
Upscaling motor protein activity to perform work in man-made devices has long been an ambitious goal in bionanotechnology. The use of hierarchical motor assemblies, as realized in sarcomeres, has so far been complicated by the challenges of arranging sufficiently high numbers of motor proteins with nanoscopic precision. Here, we describe an alternative approach based on actomyosin cortex-like force production, allowing low complexity motor arrangements in a contractile meshwork that can be coated onto soft objects and locally activated by ATP. The design is reminiscent of a motorized exoskeleton actuating protein-based robotic structures from the outside. It readily supports the connection and assembly of micro-three-dimensional printed modules into larger structures, thereby scaling up mechanical work. We provide an analytical model of force production in these systems and demonstrate the design flexibility by three-dimensional printed units performing complex mechanical tasks, such as microhands and microarms that can grasp and wave following light activation.
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