Organs-on-Chips and 3D-Cultures: Technologies and Approaches Agenda

Conference Registration, Materials Pick- and Continental Breakfast in the Exhibit Hall

Coffee Break and Networking in the Exhibit Hall

Networking Lunch, Discussions with Exhibitors and View Posters

Reality check – Industrial Development of Organ-on-a-Chip Systems
Holger Becker, Chief Scientific Officer, Microfluidic ChipShop GmbH, Germany

While in recent years the number of academic publications concerning organ-on-a-chip devices has skyrocketed, the transfer of such approach into commercial products faces a variety of specific challenges. The first challenge usually lies in the material selection. Novel materials such as elastomeric thermoplastics materials allow a scale-up in manufacturing while having physical properties closer to the frequently used elastomers in academia. In many applications, specific surface functionalization steps are required for cell adhesion. Again, the scalability and cost are relevant parameters. Finally, further back-end processing steps such as assembly and integration complement the process chain. We will present examples for scalable manufacturing technologies in cell-based devices and discuss hurdles and barriers for commercialization.

Supporting Angiogenic Development in Organ Printing
William G Whitford, Life Science Strategic Solutions Leader, DPS Group, United States of America
Michael Golway, President & CEO, Advanced Solutions, Inc., United States of America

Larger tissues require angiogenic development for successful in vivo grafting.  Development of functional vascularization requires optimized cell preparation, printing technologies, bioinks and maturation procedures.

Microfluidic Flowcell Systems and Platform Technologies as Versatile Carriers and Interfacing Solutions for Organ-on-a-Chip Applications
Herman Blok, Business Development Manager, Micronit Microtechnologies, Netherlands

An overview will be given of developed microfluidic platform technology and interfacing solutions for a number of Organ-on-a-Chip (OOC) applications. As the scope and diversity of OOC and 3D-bioprinting applications is growing rapidly there is a need for consolidation and standardization in the control, containment and interfacing solutions for microfluidic chips and devices.  We have developed various scalable Design-For-Manufacturability (DFM) concepts for such OOC applications, varying from resealable devices to fully integrated microtiter plate format culturing tools. The concepts are tested and validated in the field by end-users. Here, we demonstrate their use and applicability as versatile, flexible and enabling R&D tools for prototyping and (further) development of OOC applications.

A Benchtop Microfluidic Culture Platform for Culturing Tissue with Live Imaging Under Physiological Flow Conditions On a Laboratory Bench
Thomas Corso, Chief Technical Officer, CorSolutions, United States of America

To date, tissue culture with live imaging under physiological flow conditions is challenging.  To address these difficulties CorSolutions has developed a Benchtop Microfluidic Culture Platform for studying tissue culture under physiologically relevant conditions outside of an incubator.  This flexible, universal platform incorporates fluidic interconnects, pulse-free fluid delivery pumps, and optics to offer a simple alternative to the conventional incubator.  The Benchtop Microfluidic Culture Platform can interface a variety of microfluidic devices to the macro world.  To evaluate the platform, perfused microvessels consisting of human umbilical cord vascular endothelial cells, expressing green fluorescent protein, were cultured.  The approach allowed for live cell imaging while subjecting the culture to the physiological shear stress of 15 dynes/cm², throughout the 3 day experiment.  The results showed an unexpected active migration of cells both with and against the flow, including traversal of the branching channels, and their eventual alignment and polarization in the direction of flow.  The live imaging revealed cell behavior that had never before been observed as endothelial cells had been believed to be quiescent, undergoing mitosis only once every one to two years.  Although the implications of the observed cell migrations are not yet known, it is clear that the Benchtop Microfluidic Culture Platform is a tool with tremendous potential for probing cellular behavior.

Standard Tools for Biology
Danny Cabrera, CEO, Biobots Inc, United States of America

Biology is the most sophisticated manufacturing technology that we know of. If we could control life, we could cure disease, eliminate the organ waiting list, revert climate change and push life to other planets. However, our ability to engineer living systems has been restricted by the lack of standard tools that exist for manipulating biology. BioBots is addressing this need by creating a standard suite of digital biofabrication tools. Together with our partners and clients, we are blending biology with robotics and software to re-imagine the modern laboratory and push the human race forward.

Coffee Break and Networking

Panel Discussion Focusing on Challenges and Opportunities in the Organs-on-Chip Space Moderated by Dr. David Hughes, CN Bio Innovations Ltd.

Networking Cocktail Reception for All Delegates, Speakers, Sponsors and Exhibitors: Enjoy Beer, Wine, Appetizers and a View of the Charles River and Boston from the 15th Floor Conference Center

Close of Day 1 of the Conference

Morning Coffee, Breakfast Pastries, and Networking

Digital Magnetophoresis for Rare Cell Collection and their Logical Manipulation
Cheolgi Kim, Professor, Daegu Gyeongbuk Institute of Science and Technology (DGIST), Korea South

The ability to manipulate individual cells has profound applications for gene sequencing, single cell analysis for their heterogeneity based on cell separation technology. Even though, various single cell platforms are exit, it is still challenge to collect rare cells and their digital manipulation in large-scale. Here, we demonstrate a class of integrated magnetic track circuits for executing sequential and parallel, timed operations on an ensemble of single particles and cells. The magnetic tracks are fabricated by lithographic technology. These magnetic tracks used for the passive control of cells/particles similar to electrical conductor, diodes and capacitor. When the magnetic tracks are combined into arrays and driven by rotating magnetic field, the single cells are precisely control for multiplexed analysis. In addition, the concentric cell translocation and separation were performed by the assembly of this magnetic track into a novel architecture, resembled with spider web network, where all the cells are concentrated into one position and then transported to apartments for the single cell analysis.

Raman Imaging and Beat Profiling of the Pharmacological Reaction of Neonatal Rat Cardiomyocytes in a Centrifugal Microfluidic Chip
Wilfred Espulgar, Research Fellow, Osaka University, Japan

Raman images and beat profiles of neonatal rat cardiomyocytes trapped in a centrifugal microfluidic chip applied for pharmacological reaction study.

Inflammation on a Chip
Daniel Irimia, Associate Professor, Surgery Department, Massachusetts General Hospital (MGH), Shriners Burns Hospital, and Harvard Medical School, United States of America

Technology Spotlight:
Tissue Engineered Vascularized Tumor Micro-environments for Preclinical Testing of Anticancer Therapeutics and Toxicology
Henning Mann, Senior Research Scientist, Nortis, Inc.

Nortis provides microfluidic chips for tissue engineering 3D-vascularized tissue micro-environments.  Endothelial vessels induced to sprout in response to growth factors create a vascular network that invades tumor tissue. The model can be used to test anticancer therapeutics but can also be applied to the generation of organ-specific vascular and tissue micro-environments.

Technology Spotlight:
3D Printing in Biocompatible Polymers
Richard Gray, Regional Director, Blacktrace, Inc.

3D printers must overcome two significant challenges to address applications in Life Science – first, being able to print using biocompatible FDA approved materials, and second, being able to print leak-proof microfluidic channels and structures. This presentation describes development of Dolomite’s Fluidic Factory, which can print fluidically sealed parts in COC in minutes. Key product technologies will be described, and examples of applications in life sciences will be given.

Coffee Break and Networking in the Exhibit Hall

Advanced Integrated Optical Oxygen and pH Sensors for Organ-on-Chip Applications
Torsten Mayr, Associate Professor, Leader-Applied Sensors, Graz University of Technology Austria, Austria

Integrated optical oxygen and pH sensors are presented enabling monitoring of oxygen content and pH changes in microfluidic cell cultures or organ on chips with a high precision read-out.

Networking Lunch in the Exhibit Hall: Visit Exhibitors and Poster Viewing

Combining Microtissue Spheroids and Integrated Microfluidic Technology for Parallelized Micro-physiological Systems
Olivier Frey, Vice President Technologies and Platforms, InSphero AG, Switzerland

The presentation will focus on recent developments and experimental results combining spherical microtissues with integrated microfluidic technology for creating microphysiological multi-tissue systems. I will highlight, why spheroids as a 3D cell culturing model are suitable for such application and how we implemented their integration into microfludic culturing systems for automated parallelized assays bearing high flexibility in application, robustness and usability. Further, the implementation of microsensors and pumps will be presented and discussed.

Reconstitution and Visualization of Tumors-on-Chip for Precision Medicine
Maria Carla Parrini, Senior Research Engineer, Institut Curie, France

Tumor microenvironments are ecosystems composed of a variety of cell types positioned in complex physicochemical contexts. We generated microfluidic devices in which highly-controlled cell co-cultures reconstituted a breast tumor ecosystem (Her2+ sub-type), containing cancer cells, cancer-associated fibroblasts, endothelial cells, and immune cells. We succeeded in recapitulating on these tumors-on-chip the immune-dependent systemic response to a drug used in clinic, the Trastuzumab monoclonal antibody (Herceptin^®). This approach provides a novel experimental system to understand the complex effects of Trastuzumab on the tumor microenvironment and, very importantly, to investigate its resistance mechanisms. We are currently working toward the personalization of these tumors-on-chip by the introduction of patient-derived cells in the perspective of personalized diagnostic and precision medicine.

Human Disease Model to Study Vascular Healing of Coronary Arteries
Volkert van Steijn, Assistant Professor, Delft University of Technology, Netherlands

Cardiovascular disease, the leading cause of death in the world, is often treated by drug eluting stents (DES) to re-open blocked arteries. However, stents damage the artery wall leading to scar formation and delayed healing. Goal: To develop an in vitro model of diseased arterial wall allowing serial and longitudinal in vitro screening of new treatment modalities. Approach: The device consists of two parallel microfluidic channels separated by a thin porous polymeric membrane. Endothelium is grown on one side and smooth muscle cells contralateral. Once the endothelium is confluent and the thickness of the smooth muscle cell layer resembles a thin fibrous cap (65 micrometer), a wound is created by laser ablation and DES treatment is mimicked. Then, using time-lapse confocal microscopy, endothelial and smooth muscle cell responses are revealed. Results: A thorough analysis is presented on the development of the fibrous cap inside the microfluidic device and it is shown how the thickness of the smooth muscle layer increases in time over a period of 28 days. Then, it is shown how to create a wound of controlled size and shape in the endothelium and how the endothelial and smooth muscle cells repair the wounded area.

Close of Track