Difference between revisions of "Team:SUSTech Shenzhen/Description"

m
Line 8: Line 8:
 
= Inspiration =
 
= Inspiration =
  
The ability to hear is one of most essential ways for us to interact with the world. Without this ability, a lot of joy could have been taken away from one's life. However, there are 360 million hearing-impaired people around the world, accounting for 5% of the world’s total population.<ref>Oishi, N.; Schacht, J. (June 2011). "Emerging treatments for noise-induced hearing loss". Expert opinion on emerging drugs. 16 (2): 235–45. PMID 21247358.</ref> In China, approximately one in six people has some hearing impairment, where more than 20% of them are completely incapable of hearing.
+
Hearing is an essential way for us to interact with the outside world. It is the most element communication tools for form the societies. However, there are 360 million hearing-impaired people around the world, accounting for 5% of the world’s total population.[1] In China, approximately one in six people has some degree of hearing impairment, out of which, more than 20% of them are completely incapable of hearing.
  
 
{{SUSTech_Shenzhen/quote|Suddenly, the audible world comes to an end. Demonic buzzing replaced the ambient sound I have been hearing for years.|Fan Jiang<ref>Our team member Fan Jiang has a history of hearing loss in his childhood at age 5, which took the audible world away from him for half a year.</ref>}}
 
{{SUSTech_Shenzhen/quote|Suddenly, the audible world comes to an end. Demonic buzzing replaced the ambient sound I have been hearing for years.|Fan Jiang<ref>Our team member Fan Jiang has a history of hearing loss in his childhood at age 5, which took the audible world away from him for half a year.</ref>}}
Line 14: Line 14:
 
Despite this serious situation, hearing loss is still categorized as "incurable" for most of the patients.<ref>Nakagawa, Takayuki (2014). "Strategies for developing novel therapeutics for sensorineural hearing loss". Frontiers in Pharmacology. 5. doi:10.3389/fphar.2014.00206</ref>
 
Despite this serious situation, hearing loss is still categorized as "incurable" for most of the patients.<ref>Nakagawa, Takayuki (2014). "Strategies for developing novel therapeutics for sensorineural hearing loss". Frontiers in Pharmacology. 5. doi:10.3389/fphar.2014.00206</ref>
  
The neurological and physical causes of hearing loss are complicated. Human hearing system is a complex pipeline with both mechanical and neural components. While the mechanical part can be repaired by surgical processes, cure for sensorineural hearing loss remains highly experimental and ineffective.<ref>Sun H, Huang A, Cao S. 2011. Current status and prospects of gene therapy for the inner ear. Human gene therapy 22: 1311-22</ref>
+
The physical causes of hearing loss are complicated. Human hearing system is a complex pipeline with both mechanical and neural components. While the mechanical part can be repaired by surgical processes, treatments for sensorineural hearing loss remains highly experimental and ineffective.<ref>Sun H, Huang A, Cao S. 2011. Current status and prospects of gene therapy for the inner ear. Human gene therapy 22: 1311-22</ref>
  
One ingenious invention, namely the cochlear implant, greatly changed the situation for the people with hearing impairment. This little device converts sound directly into electronic pulses recognizable by the cochlear nerve endings, the structure that passes audio information to the brain. However, such device significantly increases the probability of bacterial meningitis.<ref>Reefhuis, J., ... & Costa, P. (2003). Risk of bacterial meningitis in children with cochlear implants. New England Journal of Medicine, 349(5), 435-445.</ref> We cannot hesitate to wonder, "What if the bulky electronics can be replaced by a tiny layer of cells?".
+
One ingenious invention, namely the cochlear implant, greatly changed the landscape for the treatment. This tiny device directly converts sound into electronic pulses recognizable by the cochlear nerve endings, the structure that passes audio information to the brain. However, such device significantly increases the probability of bacterial meningitis, among other drawbacks.<ref>Reefhuis, J., ... & Costa, P. (2003). Risk of bacterial meningitis in children with cochlear implants. New England Journal of Medicine, 349(5), 435-445.</ref> We cannot hesitate to wonder, "What if the bulky electronics can be replaced by a layer of engineered cells?".
  
After putting extensive effort into researching previous literature, we gradually realized that there is a winding road awaiting our exploration. Compared to what has been done for optogenetics and chemogenetics, work done on regulating gene expression by sound, namely "audiogenetics", is like starlight to moonshine. How could we help people hear without a way to sense sound?
+
= Research Summary =
  
We decided to use synthetic biology methods to explore how cells sense mechanical stress, such as sound wave. Traditional gene expression regulation techniques, for example, optogenetics and chemical genetics, are widely used in biological science but are strongly limited by penetration depth and target specificity. Our aim is to establish a new method, namely <i>audiogenetics</i>, that can regulate gene expression accurately deep into dense tissue. We hope this new method could open a new window to a broad range of different research into our very own feelings.
+
After extensive literature review, we came to a conclusion that there is a winding road awaiting our exploration. Compared to recent accomplishments in engineering cells sensing light and chemicals, namely optogenetics and chemogenetics, there is little systematic research on engineering cells with capability of sensing sound.
  
= Research =
+
Other cells, such as blood vessel cells, could sense mechanical shear force. There are also a number of mechanical sensing ion channels can help us sensing mechanical stimuli such touch.<ref>TODO: ADD REF</ref> We hypothesize that it is possible to use synthetic biology approaches to engineer non sensory neuron to detect different aspects of sound, such as frequency and intensity. Our project is consistent of three aims: 1) Establishing the systematic characterization tools to analyze the response of CHO cell to mechanical signals; 2) Establishing engineered CHO cell lines with synthetic circuit containing mammalian mechanosensitive Piezo1 channel or transient receptor potential channel 5 (TRPC5), and quantitatively characterize the different mechanical response of the two cell lines; 3) Developing platform for further improvement of the mechanical sensing ion channels with directed evolution. We'd like to call the ensemble of the methodology as audiogenetics.
  
Here we designed a new way called audiogenetics, to precisely and nontoxically regulate the gene expression in cells. It used a membrane mechanosensitive channel, transient receptor potential channel 5 (TRPC5), and mammalian mechanosensitive Piezo1 channel, to transform the audio wave energy as the extracellular input signal into intracellular downstream signal. Also, we quantitatively examine the sensibility of TRPC5 and Piezo to mechanical stress by using microfluidics and hypoosmolarity.
+
Mechanosensitive channels open-and-close in response to various mechanical stress, which in turn allow for extracellular cations, such as calcium, to enter and depolarize the cell. Although not well studied <ref> did anyone publish anything on sound wave activation Piezo1 or TRPC5?</ref>, they are also likely to transduce the audio wave energy as the extracellular input signal into intracellular downstream signals. Can they transduce these transient stimuli into stable gene expression? To study all of these, we first stably integrate synthetic circuit including, tunable expression of MS channels, genetic calcium sensor and calcium sensing gene expression cassette into CHO cell genome. The calcium sensor activities was measured and validated with live cell fluorescent microscopy using ionomycin as positive stimulus. The downstream pNFAT reported was validated with chronic sound stimulation of cells expression Piezo1.
 +
 
 +
The second question is that, can the widetype and engineered CHO cell sense mechanical stress differently? After a lot of trial-and-error, we established three mechanical stimulation systems: 1) hypoosmolarity shock with transient tunable osmatic pressure; 2) tunable shear force with customized microfluidics chip; 3) piezo-driven sound stimulation cell culture chamber with tunable frequency and amplitude. To our surprise, our data suggested that, they do sensor different mechanical stress significantly differently.
 +
 
 +
Although the time is very limited, we also start engineer the TRPC5 to sense different sound parameters. We deviced a directed evolution method using selection of mutation library from functional sound sensing CHO cells. It is a iterative approaches consist of 1) random mutate putative mechanical sensing domain of the TRPC5 channel proteins, 2) integrate single copy into the identical locus of CHO cells, 3) selection of the CHO cells expression TRPC5 mutant library with downstream NFAT promoter driven YFP expression.
 +
 
 +
In addition to be used to engineering synthetic hearing cells for different sound, audiogenetics could also provide us with new synthetic biology tools, alternative to chemogenetics and optogenetics tool for research tools, due to its essential advantages, deep tissue penetration, temporal and submilimeter spatial resolution. It could also be used in cell replacement therapy such as modulating the physiology or gene expression of transplanted cells in vivo.
  
To make TRPC5 more sensitive to mechanical stress, we use protein engineering by evolution to get a mutated sTRPC5 (super TRPC5) with a high sensitivity to mechanical stress. The downstream signal is calcium ion, which is a second messenger in cells and we use calcium indicator (R-GECO) to quantify the intracellular calcium using live cell image. Cytosolic calcium regulates a series of phosphorylation and we know that it can induce specific promoters (PNFAT) transgene expression. Finally, we use GFP as the output signal to quantitatively analyze the regulatory ability of audiogenetics.
 
  
 
<html><a href="/Team:SUSTech_Shenzhen/Design" class="btn btn-success">Learn More</a></html>
 
<html><a href="/Team:SUSTech_Shenzhen/Design" class="btn btn-success">Learn More</a></html>

Revision as of 17:07, 18 October 2016

Team SUSTC-Shenzhen

Description

Project

Inspiration

Hearing is an essential way for us to interact with the outside world. It is the most element communication tools for form the societies. However, there are 360 million hearing-impaired people around the world, accounting for 5% of the world’s total population.[1] In China, approximately one in six people has some degree of hearing impairment, out of which, more than 20% of them are completely incapable of hearing.

Suddenly, the audible world comes to an end. Demonic buzzing replaced the ambient sound I have been hearing for years.

Despite this serious situation, hearing loss is still categorized as "incurable" for most of the patients.[2]

The physical causes of hearing loss are complicated. Human hearing system is a complex pipeline with both mechanical and neural components. While the mechanical part can be repaired by surgical processes, treatments for sensorineural hearing loss remains highly experimental and ineffective.[3]

One ingenious invention, namely the cochlear implant, greatly changed the landscape for the treatment. This tiny device directly converts sound into electronic pulses recognizable by the cochlear nerve endings, the structure that passes audio information to the brain. However, such device significantly increases the probability of bacterial meningitis, among other drawbacks.[4] We cannot hesitate to wonder, "What if the bulky electronics can be replaced by a layer of engineered cells?".

Research Summary

After extensive literature review, we came to a conclusion that there is a winding road awaiting our exploration. Compared to recent accomplishments in engineering cells sensing light and chemicals, namely optogenetics and chemogenetics, there is little systematic research on engineering cells with capability of sensing sound.

Other cells, such as blood vessel cells, could sense mechanical shear force. There are also a number of mechanical sensing ion channels can help us sensing mechanical stimuli such touch.[5] We hypothesize that it is possible to use synthetic biology approaches to engineer non sensory neuron to detect different aspects of sound, such as frequency and intensity. Our project is consistent of three aims: 1) Establishing the systematic characterization tools to analyze the response of CHO cell to mechanical signals; 2) Establishing engineered CHO cell lines with synthetic circuit containing mammalian mechanosensitive Piezo1 channel or transient receptor potential channel 5 (TRPC5), and quantitatively characterize the different mechanical response of the two cell lines; 3) Developing platform for further improvement of the mechanical sensing ion channels with directed evolution. We'd like to call the ensemble of the methodology as audiogenetics.

Mechanosensitive channels open-and-close in response to various mechanical stress, which in turn allow for extracellular cations, such as calcium, to enter and depolarize the cell. Although not well studied [6], they are also likely to transduce the audio wave energy as the extracellular input signal into intracellular downstream signals. Can they transduce these transient stimuli into stable gene expression? To study all of these, we first stably integrate synthetic circuit including, tunable expression of MS channels, genetic calcium sensor and calcium sensing gene expression cassette into CHO cell genome. The calcium sensor activities was measured and validated with live cell fluorescent microscopy using ionomycin as positive stimulus. The downstream pNFAT reported was validated with chronic sound stimulation of cells expression Piezo1.

The second question is that, can the widetype and engineered CHO cell sense mechanical stress differently? After a lot of trial-and-error, we established three mechanical stimulation systems: 1) hypoosmolarity shock with transient tunable osmatic pressure; 2) tunable shear force with customized microfluidics chip; 3) piezo-driven sound stimulation cell culture chamber with tunable frequency and amplitude. To our surprise, our data suggested that, they do sensor different mechanical stress significantly differently.

Although the time is very limited, we also start engineer the TRPC5 to sense different sound parameters. We deviced a directed evolution method using selection of mutation library from functional sound sensing CHO cells. It is a iterative approaches consist of 1) random mutate putative mechanical sensing domain of the TRPC5 channel proteins, 2) integrate single copy into the identical locus of CHO cells, 3) selection of the CHO cells expression TRPC5 mutant library with downstream NFAT promoter driven YFP expression.

In addition to be used to engineering synthetic hearing cells for different sound, audiogenetics could also provide us with new synthetic biology tools, alternative to chemogenetics and optogenetics tool for research tools, due to its essential advantages, deep tissue penetration, temporal and submilimeter spatial resolution. It could also be used in cell replacement therapy such as modulating the physiology or gene expression of transplanted cells in vivo.


Learn More

Formula of Feeling Sound

Sound = Wave = Vibration NFAT + Gene = Regulation IonChannel + = Feeling CaInflux 2+ Direct Evolution Measurement Plasmid Construction

References

  1. Our team member Fan Jiang has a history of hearing loss in his childhood at age 5, which took the audible world away from him for half a year.
  2. Nakagawa, Takayuki (2014). "Strategies for developing novel therapeutics for sensorineural hearing loss". Frontiers in Pharmacology. 5. doi:10.3389/fphar.2014.00206
  3. Sun H, Huang A, Cao S. 2011. Current status and prospects of gene therapy for the inner ear. Human gene therapy 22: 1311-22
  4. Reefhuis, J., ... & Costa, P. (2003). Risk of bacterial meningitis in children with cochlear implants. New England Journal of Medicine, 349(5), 435-445.
  5. TODO: ADD REF
  6. did anyone publish anything on sound wave activation Piezo1 or TRPC5?

Made by from the iGEM team SUSTech_Shenzhen.

Licensed under CC BY 4.0.