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{{Franconia}} | {{Franconia}} | ||
<html> | <html> | ||
− | <style> | + | <style> |
− | + | ||
− | + | .banner-heading > h3 { | |
− | + | color: white !important; | |
− | + | } | |
− | + | ||
− | + | /* Turn off parallax scrolling for tablets and phones. Increase/decrease the pixels if needed */ | |
− | } | + | @media (max-width: 1024px) { |
− | + | .banner { | |
− | . | + | background-attachment: scroll; |
− | + | } | |
− | + | ||
− | + | .banner h1 { | |
− | @media (max-width: 1024px) { | + | font-size: 180%; |
− | + | font-weight: 100; | |
− | background- | + | } |
− | } | + | } |
− | + | ||
− | + | .light { | |
− | + | text-align: center; | |
− | + | } | |
− | + | ||
− | + | #headervideo { | |
− | + | opacity: 0.3; | |
− | + | object-fit: fill; | |
− | + | } | |
− | } | + | |
− | + | .banner { | |
− | . | + | height: initial !important; |
− | + | ||
− | + | } | |
− | } | + | |
− | + | .banner-button { | |
− | . | + | color: white; |
− | margin: | + | margin-top: 30px; |
− | + | cursor: pointer; | |
− | + | padding: 15px; | |
− | + | border: 1px solid white; | |
− | + | border-radius: 10px; | |
− | + | display: inline-block; | |
− | + | font-size: larger; | |
− | } | + | font-weight: 500; |
− | + | } | |
− | + | ||
− | + | @media (max-width: 768px) { | |
− | } | + | .banner-heading h3 { |
− | + | font-size: x-large; | |
− | + | } | |
− | @media (max-width: | + | } |
− | + | ||
− | + | @media (max-width: 1024px) { | |
− | } | + | #headervideo { |
− | + | display: none !important; | |
− | . | + | } |
− | + | ||
− | + | .banner { | |
− | } | + | background-image: url("/images/Banner/DNAImage.png"); |
− | } | + | height: 65vh !important; |
− | + | box-shadow: inset 0 0 0 2000px rgba(50, 71, 85, 0.7); | |
− | . | + | top: -3px; |
− | + | width: 100vw; | |
− | } | + | background-color: var(--tint-color); |
− | + | background-attachment: fixed; | |
− | + | background-position: center; | |
− | + | background-repeat: no-repeat; | |
− | + | background-size: cover; | |
− | + | ||
− | + | } | |
− | + | ||
− | + | .banner .banner-heading { | |
− | + | top: initial !important; | |
− | + | } | |
− | + | } | |
− | + | ||
− | + | .center.home { | |
− | + | margin-bottom: 5%; | |
− | </style> | + | } |
− | + | ||
− | + | .center.home > div > a > div > img { | |
− | <div class=" | + | margin-bottom: 10%; |
− | <canvas style="width: 100%; height: 100%; z-index: -1;"></canvas> | + | border-radius: 10% 100% 100% 100%; |
− | <div class=" | + | border: 2px solid var(--tint-color); |
− | + | } | |
− | + | ||
− | + | .center.home > div > a > div > h4 { | |
− | </div> | + | font-weight: 300 !important; |
− | </div> | + | } |
− | + | ||
− | <div class=" | + | @media screen and (max-width:767px) { |
− | + | .col-sm-3.lastStep { | |
− | + | margin-bottom: 30% !important; | |
− | + | } | |
− | + | } | |
− | + | ||
− | + | ||
− | + | </style> | |
− | + | ||
− | + | <div class="banner"> | |
− | + | . <!--- <canvas style="width: 100%; height: 100%; z-index: -1;"></canvas> --> | |
− | + | <video muted id="headervideo" src="https://static.igem.org/mediawiki/2017/b/b5/T--Franconia--DNA_background_c.mp4" style="width:100%; height:100%" autoplay | |
− | + | loop></video> | |
− | + | <div class="banner-heading"><h1>B.E.A.M.</h1> | |
− | + | <h3>Biocompatible Elastic Artificial Muscle</h3> | |
− | + | <div class="banner-button">Beam me up!</div> | |
− | + | </div> | |
− | + | ||
− | + | </div> | |
− | + | ||
− | + | <div class="container-fluid"> | |
− | + | <div class="content"> | |
− | + | <h3>Abstract</h3> | |
− | + | <p> | |
− | + | The development of artificial muscles attracts wide interest for industrial and medical | |
− | + | applications. Regarding manufacturing, robotic devices with synthetic muscles are able to | |
− | + | handle softer materials more precisely. Moreover, artificial musculatures in medical | |
− | + | prostheses can improve the wearing comfort while conveying a rather natural feeling. | |
− | + | Currently, muscle-like contractions can be obtained by capacitor systems or by molecular | |
− | + | machines incorporating tissue. This project aims to replace the common materials in both | |
− | + | branches by biological tissue. While increasing ecological friendliness and the compatibility | |
− | + | with human tissue, those fabricated compositions can compete with human biological | |
− | + | material. <br> <br> | |
− | </div> | + | Like a capacitor, the dielectric elastomer actuator (DEA) comprises two lightweight and |
− | + | flexible electrodes separated by an insulating elastomeric layer. In a first set of experiments, | |
− | <script> | + | the elastomer layers in the capacitor-based muscle need to be replaced by appropriate protein |
− | + | structures. P-Pili with their excellent elastic properties and proteins with high amounts of | |
− | $(document).ready(function() { | + | helical secondary architecture are to be tested for this approach. In a next step, the currently |
− | + | used light weighted graphene or carbon nanotube layers need to be replaced by the Pili to | |
− | + | provide conductivity and flexibility comparable to the carbon nanotubes. Both fibril types can | |
− | + | be easily expressed in Geobacter sulflurreducens and Escherichia coli in a large scale, which | |
− | + | makes the overall system extremely feasible since one organism can provide the whole | |
− | + | material. <br> <br> | |
− | + | </p> | |
− | + | <div class = "center home"> | |
− | + | <div class="content"> | |
− | } | + | <h3>Method 1</h3> |
− | + | </div> | |
− | + | <div class = "row"> | |
− | }) | + | <a href="/beam.php#"> |
− | }) | + | <div class = "col-sm-3"> |
− | </script> | + | <h4>Step 1</h4> |
− | + | <img src = "/images/Home/BioBricks.png"> | |
+ | <div> | ||
+ | <p>Protein Building Blocks</p> | ||
+ | </div> | ||
+ | </div> | ||
+ | </a> | ||
+ | <a href="/beam.php#"> | ||
+ | <div class = "col-sm-3"> | ||
+ | <h4>Step 2</h4> | ||
+ | <img src = "/images/Home/Black:Blue.png"> | ||
+ | <div> | ||
+ | <p>Tissue is formed</p> | ||
+ | </div> | ||
+ | </div> | ||
+ | </a> | ||
+ | <a href="/beam.php#"> | ||
+ | <div class = "col-sm-3"> | ||
+ | <h4>Step 3</h4> | ||
+ | <img src = "/images/Home/NanoShit.png"> | ||
+ | <div> | ||
+ | <p>Pilis/Carbon Nano Tubes are added</p> | ||
+ | </div> | ||
+ | </div> | ||
+ | </a> | ||
+ | <a href="/beam.php#"> | ||
+ | <div class = "col-sm-3 lastStep"> | ||
+ | <h4>Step 4</h4> | ||
+ | <img src = "/images/Home/Finished.png"> | ||
+ | <div> | ||
+ | <p>Artificial Muscle is created</p> | ||
+ | </div> | ||
+ | </div> | ||
+ | </a> | ||
+ | </div> | ||
+ | <div class="content"> | ||
+ | <h3>Method 2</h3> | ||
+ | </div> | ||
+ | <div class = "row"> | ||
+ | <a href="/beam.php#"> | ||
+ | <div class = "col-sm-3"> | ||
+ | <h4>Step 1</h4> | ||
+ | <img src = "/images/Home/Bricks.png"> | ||
+ | <div> | ||
+ | <p>Protein Building Blocks</p> | ||
+ | </div> | ||
+ | </div> | ||
+ | </a> | ||
+ | <a href="/beam.php#"> | ||
+ | <div class = "col-sm-3"> | ||
+ | <h4>Step 2</h4> | ||
+ | <img src = "/images/Home/Orange.png"> | ||
+ | <div> | ||
+ | <p>Tissue is formed</p> | ||
+ | </div> | ||
+ | </div> | ||
+ | </a> | ||
+ | <a href="/beam.php#"> | ||
+ | <div class = "col-sm-3"> | ||
+ | <h4>Step 3</h4> | ||
+ | <img src = "/images/Home/Farbstoff.png"> | ||
+ | <div> | ||
+ | <p>Azo Dye is added</p> | ||
+ | </div> | ||
+ | </div> | ||
+ | </a> | ||
+ | <a href="/beam.php#"> | ||
+ | <div class = "col-sm-3 lastStep"> | ||
+ | <h4>Step 4</h4> | ||
+ | <img src = "/images/Home/Muscle.png"> | ||
+ | <div> | ||
+ | <p>Artificial Muscle is created</p> | ||
+ | </div> | ||
+ | </div> | ||
+ | </a> | ||
+ | </div> | ||
+ | </div> | ||
+ | <p> | ||
+ | Another tissue with muscle-like contractions will be fabricated through polymers with | ||
+ | integrated molecular machines. Herein, the latter are based on azo dyes capable of having | ||
+ | their entire network contracted by light irradiation. The biopolymer matrix is fabricated by | ||
+ | Escherichia coli and consists of catcher-tag systems modified with a biotin-accepting anchor. | ||
+ | The molecular machines attach to the biopolymer tissue via biotin and biotin acceptor | ||
+ | interactions. Due to the crosslinking of the single protein strains the stiffness of the resulting | ||
+ | tissue can be adjusted accurately. <br> <br> | ||
+ | In both cases, the achieved tissues are cell-free and can immediately be adapted to the system. | ||
+ | Within the scope of the project, the construction of a DEA-prototype is planned, since the | ||
+ | realization of electrical stimuli is more feasible than through photo-induced signals. | ||
+ | </p> | ||
+ | </div> | ||
+ | </div> | ||
+ | |||
+ | <script> | ||
+ | $(document).ready(function () { | ||
+ | $('.banner-button').click(function () { | ||
+ | console.log('scrolling'); | ||
+ | $('html, body').stop().animate({ | ||
+ | 'scrollTop': $('.content').offset().top - 100 | ||
+ | }, 500, 'swing'); | ||
+ | }); | ||
+ | }) | ||
+ | |||
+ | </script> | ||
</html> | </html> | ||
{{Franconia/Footer}} | {{Franconia/Footer}} |
Revision as of 23:52, 30 October 2017
Abstract
The development of artificial muscles attracts wide interest for industrial and medical
applications. Regarding manufacturing, robotic devices with synthetic muscles are able to
handle softer materials more precisely. Moreover, artificial musculatures in medical
prostheses can improve the wearing comfort while conveying a rather natural feeling.
Currently, muscle-like contractions can be obtained by capacitor systems or by molecular
machines incorporating tissue. This project aims to replace the common materials in both
branches by biological tissue. While increasing ecological friendliness and the compatibility
with human tissue, those fabricated compositions can compete with human biological
material.
Like a capacitor, the dielectric elastomer actuator (DEA) comprises two lightweight and
flexible electrodes separated by an insulating elastomeric layer. In a first set of experiments,
the elastomer layers in the capacitor-based muscle need to be replaced by appropriate protein
structures. P-Pili with their excellent elastic properties and proteins with high amounts of
helical secondary architecture are to be tested for this approach. In a next step, the currently
used light weighted graphene or carbon nanotube layers need to be replaced by the Pili to
provide conductivity and flexibility comparable to the carbon nanotubes. Both fibril types can
be easily expressed in Geobacter sulflurreducens and Escherichia coli in a large scale, which
makes the overall system extremely feasible since one organism can provide the whole
material.
Method 1
Step 1
Protein Building Blocks
Step 2
Tissue is formed
Step 3
Pilis/Carbon Nano Tubes are added
Step 4
Artificial Muscle is created
Method 2
Another tissue with muscle-like contractions will be fabricated through polymers with
integrated molecular machines. Herein, the latter are based on azo dyes capable of having
their entire network contracted by light irradiation. The biopolymer matrix is fabricated by
Escherichia coli and consists of catcher-tag systems modified with a biotin-accepting anchor.
The molecular machines attach to the biopolymer tissue via biotin and biotin acceptor
interactions. Due to the crosslinking of the single protein strains the stiffness of the resulting
tissue can be adjusted accurately.
In both cases, the achieved tissues are cell-free and can immediately be adapted to the system.
Within the scope of the project, the construction of a DEA-prototype is planned, since the
realization of electrical stimuli is more feasible than through photo-induced signals.