The present disclosure is generally related to bioreactors for tissue engineering
One standard research tool employed in tissue engineering and biological research is the transwell membrane. These membranes are used in multiwall plates and allow culturing single and bi layers of cells with media on each side. Other methods use perfused chambers where cells or tissues are cultured on the bottom or sides of a chamber through which media is flowed. Neither of these methods allow for stacking of multiple bilayers of cells.
Disclosed herein is an apparatus comprising: an enclosure comprising a base and a top and a plate. The base and the top each comprise an interior surface which together define the interior of the enclosure. The base and the top each comprise an inlet fluid channel and an outlet fluid channel from the interior of the enclosure to the exterior of the enclosure. The plate is in the interior of the enclosure and comprises a frame having an opening, a gasket, and a biopaper spanning the opening. The plate divides the interior of the enclosure into two cavities. A portion of the biopaper is not touching the frame, the gasket, or the interior surfaces. The biopaper is fluid communication with the fluid channels.
A more complete appreciation will be readily obtained by reference to the following Description of the Example Embodiments and the accompanying drawings.
In the following description, for purposes of explanation and not limitation, specific details are set forth in order to provide a thorough understanding of the present disclosure. However, it will be apparent to one skilled in the art that the present subject matter may be practiced in other embodiments that depart from these specific details. In other instances, detailed descriptions of well-known methods and devices are omitted so as to not obscure the present disclosure with unnecessary detail.
Disclosed herein is a modular bioreactor based around stackable inserts that serve as a substrate for various culture conditions. Different tissues will require different environmental conditions including air or media exposure, as well as different cell and biomaterial arrangements. The modular system supports various configurations such as monolayer cultures and bilayer cultures with cells on either side of a single insert. Multi-layer cultures with multiple inserts having mono or bilayer cultures each as well as some inserts having the entire inter-insert space filled by hydrogel or other cell matrix/scaffolding components.
The bioreactor may be used as a platform for constructing, culturing, and studying engineered tissues. The platform is modular in that it is an assembly of pieces which can be altered to allow for the creation of specific tissue construct, culture, or monitoring or other research scenarios. Central to all configurations is a plate or insert which is the foundation of the smallest tissue block supported by the platform. The plate is a framed biopaper, a single membranous layer upon or into which single or multiple cell types can be applied via traditional or cell printing methods. The bioreactor allows for any number of these biopaper supported tissue layer inserts to be stacked, either directly or with spacers to create vacancies between layers. Perfusion of each layer is facilitated by holes and channels built into the biopaper frame, which align with fluidic channels in the bioreactor. All this is to create a flexible in vitro platform for tissue engineering and research.
The plates or inserts are framed with a rigid material that allows them to fit into a receiving area on the inside of the bioreactor, pins, rails, or other geometric fittings align the insert into a specific area in the bioreactor. This alignment allows for the insert to be coupled to microfluidic channels in the bioreactor as well as aligned to other similar inserts which can be stacked above or below. This alignment of features between layers can be used to create complex three-dimensional cell/biomaterial/environmental arrangements using any number of conventional two-dimensional cell and bio factor printing techniques. The insert may be removable with or without disassembly of the bioreactor.
The inserts may be separated by a polymer gasket or spacer that not only serves to seal the chamber, but also to create inter-insert spaces which can be filled with cell culture media, extracellular matrix components (hydrogel) and cell components.
Inserts may be biopapers such as those disclosed in U.S. Pat. No. 8,669,086, US Pat. Appl. Pub. No. 2014/0154771, and U.S. patent application Ser. No. ______ entitled “BIOPAPERS AS A SUBSTRATE FOR TISSUE CULTURE, filed by Pirlo et al. on the same day as the present application, metal or polymer frames with membranes overlaid or electrospun onto them, and may support tissue constructs including cell monolayers, bilayers, 3D hydrogels and 3D cell/hydrogel/scaffolding composites. Biopapers can be used that are degradable or non-degradable, and that have mechanical and chemical characteristics that are selected to suit the cells and tissues being cultured. The biopapers can also include electrodes.
The frames of the biopaper may also include channels which act as connecting conduits between fluid channels in the bioreactor and fluid channel/vascular constructs/media spaces in the insert, including any cell structures created on it or in the attached 3D cell/hydrogel/scaffolding composite.
The bioreactor may include windows in the top and/or the bottom over the interior, bleed chamber, inlets, or outlets for performing optic-based sensing. Optical or fluorescent methods may include sensing coupons for pH or O2.
The plate 14 divides the interior of the enclosure into two cavities on either side of the plate. The plate 14 comprises a frame 28 having an opening, a gasket 30, and a biopaper 32 spanning the opening. The biopaper 32 is positioned to be in fluid communication with the fluid channels 24, 26, that is, fluid entering each of the inlet channels may contact one side or other of the biopaper, then exit the enclosure through the outlet channels. A portion of the biopaper 32 is not touching the frame 28, the gasket 30, or the interior surfaces 20 so that fluid may contact that portion on both sides of the biopaper 32. The frame 28 and the gasket 30 may be positioned to prevent any fluid flow directly between the cavities other than through the biopaper itself, if possible. The frame 28 and the gasket 30 may be separate components are may be a unitary component.
The frame may be made of similar compatible materials as the enclosure. One suitable frame material is Cyclic Olefin Copolymer (COC, e.g. ethylene-norbornene copolymer). COC has a glass transition temperature that can be selected to allow for hot embossing of micro channels for perfusion of the supported tissue layer, but resist melting when autoclave sterilized. The gasket is also a compatible material, and also prevents fluid flow into or out of the enclosure. Polytetrafluoroethylene is one suitable gasket material.
Further components of the bioreactor may include a pair of electrodes in the base and top that are in fluid communication with either side of the biopaper. These electrodes may allow for trans-membrane electrical resistance (or trans endothelial/epithelial electrical resistance (TEER)) to be measured non-invasively and with no movement of the electrodes. These electrodes may comprise silver.
The system may further include electronics as part of the biopaper frame/biopaper plate. These electronics may allow for sensing and stimulation activity to be performed at the biopaper surfaces.
The system can be adapted to model specific tissues or create various modeling scenarios by altering the material used in the membrane component of the biopaper, as well as any other components that are applied to the biopaper. The bioreactor platform can be adapted to thick or thin tissue models by including different numbers and/or types of biopaper inserts. When the bioreactor is used to construct thick, solid, tissue constructs, by stacking multiple cell laden biopaper inserts, it may have the benefit of pre-maturation of individual layers before stacking (either in dish or in the multiple bioreactors before stacking). This can solve a long standing problem of necrosis developing in the center of thick tissue constructs where diffusional transport of oxygen, nutrients, and waste are insufficient. With this bioreactor design each layer can have a mature engineered vascular/fluidic system before stacking which aligns perfectly to the flow channels of the bioreactor frame of the biopaper insert inserted into the matched recess in the bioreactor. The perfusion system described is easily scalable to any number of inserts as through holes in the rigid frame act as the main flow conduit, and open faced channels in the rigid frame become individual fluidic branches of the main tissue as they are stacked.
The system can be used to create thin tissue constructs that model barrier tissues such as lung or the blood brain barrier where the cavities on either side of a membrane are isolated from each other via the biopaper membrane and the surrounding bioreactor and gaskets. This isolation provides for modeling barrier tissues with differing apical and basal media components, or different phases, such as liquid media and air.
The electrodes allow for continuous, highly reproducible, and non-invasive monitoring of TEER, a significant improvement over conventional TEER apparatus that have a user positioned electrode and require opening of the tissue culture environment for reading.
The rigid frame stacking system allows for high resolution alignment of layers to each other which allows for three dimensional patterns of cells and materials (biological or otherwise) to be created via two dimensional patterning and printing methods.
The rectangular form shown is used to aid in the subtractive machining method used, but other shapes could be used if the bioreactor were formed by additive or molding methods, however the basic design of a stack of framed membranes which create a fluidic manifold for perfusion of any number of layers via stacking would be retained. Size (area and depth) of chambers may be adjusted to account for desired tissue volumes, and required media/air reservoir spaces.
Obviously, many modifications and variations are possible in light of the above teachings. It is therefore to be understood that the claimed subject matter may be practiced otherwise than as specifically described. Any reference to claim elements in the singular, e.g., using the articles “a”, “an”, “the”, or “said” is not construed as limiting the element to the singular.
This application claims the benefit of U.S. Provisional Application No. 62/262,635, filed on Dec. 3, 2015. The provisional application and all other publications and patent documents referred to throughout this nonprovisional application are incorporated herein by reference.
Number | Date | Country | |
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62262635 | Dec 2015 | US |