Sara
Shakibania
a,
Mehrdad
Khakbiz
*a,
Cemile Kilic
Bektas
b,
Lida
Ghazanfari
c,
Milad Tavakoli
Banizi
a and
Ki-Bum
Lee
*b
aDivision of Biomedical Engineering, Faculty of New Sciences and Technologies, University of Tehran, North Kargar Ave., PO Box 14395-1561, Tehran, Iran. E-mail: khakbiz@ut.ac.ir
bDepartment of Chemistry and Chemical Biology Rutgers, The State University of New Jersey, Piscataway, NJ 08854, USA. E-mail: kblee@rutgers.edu
cCenter for Nanotechnology in Drug Delivery, University of North Carolina, Chapel Hill, NC, USA
First published on 8th March 2022
Early diagnosis of diseases leads to selecting the appropriate treatment method and prevention of problems, such as drug resistance. It also prevents the spread of diseases and pandemics in some cases and plays a crucial role in treating diseases. In some diseases, such as bacterial infections, effective diagnoses prevent antibiotic overuse and make such antibiotic treatments futile against infections. Additive manufacturing (AM) or 3D printing has received great attention in recent years and has been applied in a wide variety of biomedical applications, such as implants and diagnostic tools. The structures fabricated via this method are highly precise and economical and can have complex geometries, such as interconnecting channels, undercuts, and curvatures. Developing sensors and sensor arrays in a shorter time with high sensitivity is possible by applying AM fabrication approaches. Other fields such as dentistry also take advantage of 3D printing technology to ease the diagnosis process as it helps to fabricate complex structures with dimensions close to reality which cannot be achieved by any other method. In this review, recent advances in AM fabrication methods in producing rapid diagnosis tools have been discussed by providing a classification of advanced diagnostic tools using AM.
Design, System, ApplicationAdditive manufacturing (AM) has attracted growing interest for different industries. This article provides a review of fabrication of biosensors and diagnostic tools via additive manufacturing. This mini-review will provide an applicable classification of diagnostic tools fabricated by different AM methods such as fused deposition modeling, stereolithography, and selective laser melting. The application of bioprinting for designing sensors and different mechanisms such as extrusion, inkjet, and laser-based methods are studied. This mini review summarizes design principles and mechanisms and challenges in additive manufacturing to achieve high-performance sensors. Each of the AM methods results in specific properties and characteristics of the fabricated biosensor. Some parameters including the heat source type, build orientation, thickness of the layers, raster width and angle, air gap, and feed rate, which can affect systematically the properties and characterization of biosensors, are investigated in this paper. |
Technology | Vat photopolymerization | Material extrusion | Powder bed fusion (PBF) |
---|---|---|---|
Method | Stereolithography | FDM/ FFF | SLS/SLM |
Resolution (μm) | 50–200 (ref. 10) | 100–400 (ref. 11) | 50–100 (ref. 11) |
Layer thickness (μm) | <10 μm (ref. 12) | From 100 to 250 μm (ref. 12) | From 25 to 100 μm (ref. 12) |
Principle | Photo-polymerisation | Melt extrusion | Powder sintering |
Materials | Photo-curable polymers13/composites/cells10 | Polymers, ceramics, metals13/composites/cells10 | Polymers, metals, ceramics13/composites10 |
Advantages | Highly accurate | Cost-efficient14 | Highly accurate14 |
Appropriate surface finishing14 | Facile multi-material printing14 | Acceptable strength and stiffness14 | |
High resolution15 | |||
Widely commercially available | |||
Potential to process both amorphous and crystalline polymers15 | |||
Disadvantages | Time consuming due to curing and refill intervals | Poor surface finishing14 or mechanical properties compared to injection molded parts15 | Slow building process14 |
Poor mechanical properties15 | Limitation in size14 | ||
Post-processing treatments needed (surface polishing, heat treatments)15 |
Fig. 1 Schematic representation of different types of flexible biosensors on the skin (created with BioRender). |
These devices can be directly attached to the skin and report accurate and real-time measurements of biomarkers.28 These biosensors can be fabricated by different techniques such as inkjet printing, screen printing, and lift-off lithography.29
The AM technique can produce structures that are either patient-specific or hard to fabricate using other methods.31 Compared to the conventional manufacturing processes such as injection molding, AM is cost-efficient as it eliminates extra tooling and re-fixturing and does not require a skilled operator, or even a long fabrication time. Complex geometric shapes can be designed and fabricated via AM technology with no additional cost, while in the conventional methods, for the more complex geometric shapes, more expensive molds are required.32 Since traditional manufacturing processes, such as injection molding, have high start-up costs, they are better suited for mass production, whereas AM is cost and time-effective for low part numbers because no startup tooling is required. Furthermore, the amount of wasted material in the AM process is remarkably low.32 As the AM manufacturing process involves a digital environment and samples are designed in digital files that can easily be shared or altered, time bottlenecks are eliminated. Another advantage of AM over other approaches is that it reduces risks associated with the workplace.14 Hence, considering the capability of fabricating samples with high geometric complexity, low wasted material, shorter time to market,14 and better efficiency of supply chains,14 AM technology is cost-efficient.32
Recent studies have concentrated on developing more cost-efficient and less time-consuming approaches with higher sensitivity. For example, in many ELISA systems, microplates of various capacities and sizes are used for antibody immobilization, necessitating a significant amount of time for incubation and washing processes. Limited surface area to immobilize antibodies is one of the challenges which restricts the use of ELISA for low-cost diagnostics.33,34 The 3D printing approach can be used to create microwells with a greater surface area, which improves the performance of microplate ELISAs. Sharafeldin et al.34 developed ELISA in 3D-printed pipet tips. The required time for the assay decreased due to the high surface area. Moreover, the roughness of the 3D-printed surface resulted in a 15–50 times higher antibody loading capacity of the surface. This increase in loading capacity lowered the required time for the assay while the sensitivity was similar to that of conventional ELISA. Moreover, 3D printing can be a cost-efficient approach for fabrication of diagnostic tools such as ELISA. Bauer et al.35 developed a 3D-printed ELISA device for detection of malaria and compared the required cost to that of different malaria-detection platforms including other 3D-printed ELISA devices, rapid diagnostic tests, and PCR. The 3D-printed ELISA device cost less than $10 depending on the reagent and printing costs while this number for rapid diagnostic tests was around $5 and, for the PCR method, could increase to $25.
Fig. 2 Schematic representation of AM fabrication processes: (a) fused deposition modeling, (b) stereolithography and (c) selective laser melting48 (created with BioRender). |
The AM procedure consists of eight general steps: 1. conceptualization and creating a CAD model. 2. Turning to STL format. 3. Conveying to the AM device and STL file manipulation. 4. Setting up the system and equipment. 5. Fabricating the sample. 6. Withdrawal and cleaning the built part. 7. Post-treatment of the fabricated samples. 8. Application.39
Sensors fabricated via AM can be highly sensitive.42 Singh et al.33 proposed a 3D printed prototype design to improve the diagnostic performance of ELISA and achieved a 2.25-fold higher sensitivity. This higher sensitivity was attributed to the larger reaction surface area in the 3D-printed samples. In another study, Guo et al.43 developed a helical structure as a multifunctional 3D liquid sensor in which the structural feature of the printed sample resulted in excellent sensitivity and selectivity as it was capable of trapping more liquid components. Petroni et al.44 fabricated an electrochemical sensor based on a graphite/acrylonitrile butadiene styrene conductive composite. The outcomes indicated better analytical performance compared to commercial carbon black/PLA conductive filaments. This is due to the production technique, which allowed for the insertion of greater amounts of conductive material in the matrix.
The performance of the sensor (such as gauge factor and linearity) can be controlled by printing parameters during the fabrication process.45 These parameters are the printing-line directions,46 needle diameter,47 ratio of components in the composites,45 and printing speed.45 Abshirini et al.47 fabricated highly flexible strain sensors by extrusion-based 3D printing. This sensor was constructed from multi-walled carbon nanotubes (MWNTs) and polydimethylsiloxane (PDMS). The influence of the needle diameter and MWNT concentrations on sensor performance was investigated. The piezoresistive sensitivity was improved when the diameter of the needle was reduced. Because the needle diameter can potentially modify the shear flow generated during the printing process, the MWNT distributions and alignment were altered as a result. Therefore the piezoresistive sensing performance of these sensors was different. Furthermore, by decreasing the amount of the MWNTs, the piezoresistive sensitivity of the printed nanocomposites was enhanced. The piezoresistive sensing mechanism depends on the MWNT network reorganization under external load and an appropriate amount of MWNTs resulted in an effective connection of MWNTs which consequently led to higher sensitivity to external loads. Vu et al.46 studied the effects of the printing-line directions (45°, 90°, 180°) on the performance of a strain sensor fabricated via the FDM method. The results showed that all three samples had acceptable performance in terms of sensitivity (GF) with the sample printed at 45° exhibiting the highest GF among the samples. The effect of other parameters such printing speed has been also studied. A change in the printing speed altered the line width of the 3D-printed sensor.45
In 2017, Gaal et al.50 used FDM techniques to fabricate biosensors composed of integrated, sealed and transparent polylactic acid (PLA) microchannels. The highlighted features of this construct were its appropriate transparency and reasonable price, the availability of raw material (PLA), the printing of microchannels without destroying the structures, and also the ease of combining other materials during the process. By way of illustration, pliable interdigitated electrodes were placed in a microfluidic e-tongue that could detect the basic tastes below the human threshold. Microfluidic devices is consist of polydimethylsiloxane (PDMS) because of its optical transparency, chemical inertness, non-toxicity, and gas permeability. However, microfluidic device production using PDMS has limitations, such as the cost, handling, and additional step requirements. Therefore, 3D printing to fabricate microfluidic biosensing devices enables the use of a wide range of materials and produces complex structures by avoiding multi-step processing. In 2018, Palenzuela et al.51 developed highly sensitive graphene-based electrodes for electrochemical sensing using the FDM method. They 3D-printed ring- and disc-shaped electrodes and used different redox probes (ferrocene monocarboxylic acid, K3Fe(CN)6:K4Fe(CN)6, ascorbic acid, FeCl3, and Ru(NH3)6Cl3) to study the electrochemical performance of the probes. They reported increased electroactivity by a simple activation protocol, which includes DMF-assisted limited dissolution of the insulating polymer polylactic acid. Marzo et al. (2020)52 also employed graphene and PLA to develop an enzymatic biosensor using the FDM approach in another study. The biosensors were produced by horseradish peroxidase (HRP) immobilization to create electrostatic interactions for H2O2 detection, and their results showed that the direct electron transfer of immobilized HRP was highly efficient. They further modified the biosensor by applying gold nanoparticles (AuNPs) to facilitate heterogeneous electron transfer and reported an enhanced biosensor performance. In 2020, Cardoso et al.53 developed other graphene–PLA (G–PLA) based amperometric biosensors for detecting glucose in biological fluids. The glucose level was measured using glucose oxidase and ferrocene-carboxylic acid (FCA) at a 15 μmol L−1 detection limit. They could also modify the surface of the same system (by solvent immersion and mechanical polishing) to detect nitric acid and uric acid to analyze saliva and urine. The G–PLA sensors developed via the FDM approach are flexible, biodegradable, and biocompatible. Furthermore, these types of biosensors can be fabricated on a large scale with various dimensions at a low cost. FDM techniques can also be used for disease/injury diagnosis purposes. Frizziero et al. (2019)54 reported the use of computed axial tomography (CAT) data which are converted into 3D-printed models, and these models are used to characterize the anatomical structure of fractures and lesions to provide a complete pre-surgery evaluation.
Aerosol jet printing (AJP) is a type of direct-write printing working in a contactless manner by using a directed aerosol stream where the polymer is deposited on the substrate at 1–5 mm offsets. AJP can fabricate fine features on complex substrates that generally cannot be reached by any physical nozzles and can be used in diverse applications, such as fabricating active and passive electronic components, actuators, and sensors.55 In 2016, Yang et al.56 developed silver microelectrode arrays (MEAs) using AJP techniques at a 15 μm resolution. The developed sensor was successfully applied to detecting hydrogen peroxide and glucose levels as model analytes to illustrate the system's performance. This study shows the potential of AJP as a fabrication tool for custom-shaped low-cost microelectrode arrays for a wide range of biosensor applications, including touch sensing, bio-sensing, and strain sensing. In 2018, Zachariah et al.57 reported the use of AJP to develop flexible hybrid electronics (FHE) that are wearable, comforting the human body, and light. For this purpose, they employed a silver nanoparticle (AgNP)-based ink and reported that the produced electronics could extend over 10 times their primary length without losing conductivity.58
In 2019, Kuo et al.60 developed a microfluidic device based on a stereolithography approach using low molecular weight poly(ethylene glycol) diacrylate (MW = 258) at sub-millimeter resolution. They reported the production of complex 3D microfluidic devices such as an active micro-mixer with pneumatic micro-valves and microchannels with a high aspect ratio (37:1), and this resolution is not available in any other conventional rapid prototyping methods. These types of complex microfluidic devices can be applied to many different research areas, including patch-clamp chips, biosensors, organ-on-a-chip, and tumor-on-a-chip.
Miller et al.61 (2011) investigated inorganic–organic hybrid microneedle-shaped materials for transdermal biosensor applications using micro-mirror device-based stereolithography instruments. The sensing mechanisms are placed in the perforation of the microneedles, and the carbon fiber electrodes are located within the hollow microneedle array created by the lithography instrument (Fig. 3). Their studies showed that the microneedles were intact after puncturing into cadaver skin. The performance of the developed ion-selective electrodes was evaluated by chemically modifying the carbon fibers to allow the detection of molecules, such as ascorbic acid and hydrogen peroxide, and measuring the current electrochemically.
Fig. 3 Schematic illustration of the hybrid microneedle developed by Miller et al.61 |
In the same year, Narayanan et al.62 fabricated a dual-mode electrochemical biosensor using the SLA technique to diagnose glucose and H2O2. The developed structure was made of tungsten coated with gold nanoparticles (AuNPs) and gold micro-wire electrodes coated with colloidal platinum (colloidal-Pt). AuNPs and colloidal-Pt acted as a support matrix to immobilize the horseradish peroxidase (HRP) and the non-enzymatic glucose biosensor, respectively. This platform was capable of identifying both glucose (with a linear range of 0.5 mM to 8 mM) and H2O2 (linearity up to 70 μM) simultaneously. This product can be considered a potential device for real-time identification of glucose and H2O2 in clinical, biological, and environmental applications.
SLM is a very suitable approach in the medical and dental areas as it allows the production of complex geometries and individualized models. Moreover, multiple parts can be fabricated in a single run, enabling mass production.65 In 2007, Vandenbroucke et al.65 investigated the effect of the SLM parameters (material, surface post-treatment, the thickness of layers, the angle of slope, and the variance between the upper and lower surfaces) on two biocompatible metal alloys: Ti–6Al–4V and Co–Cr–Mo to be used as a dental prostheses. The results confirmed that optimized SLM factors resulted in achieving a part density of up to 99.98% for titanium. The printed parts were shown to have appropriate strength and stiffness, corrosion behavior, and process precision for medical or dental applications.
Kwon et al.66 used the SLS approach to fabricate copper nanoparticle thin films onto a polymer substrate and obtained a flexible, conductive, and transparent material. The method demonstrated that Cu, which normally suffers from severe oxidation, can be sintered rapidly at low annealing temperatures with significant oxidation suppression. Their results suggest that copper-based flexible electronics can be produced onto plastic substrates using the SLS technique.
Table 2 shows a summary of developed diagnosis tools via additive manufacturing.
Year | Scientist | Material | Method | Application | Reference |
---|---|---|---|---|---|
2007 | Vandenbroucke | Ti–6Al–4V/Co–Cr–Mo | SLM | Medical application | 65 |
2017 | Gaal | PLA | FDM | e-Tongue | 50 |
2017 | Arango | Metal and metal-oxide ink | — | Engineered inks for AM | 67 |
2018 | Zacharian | Silver-based inks | 3DP | Flexible electronic substrates | 57 |
2018 | Palenzuela | PLA/G | FDM | Electrochemical sensor | 51 |
2019 | Frizziero | — | FDM | Orthopedic device | 54 |
2019 | Kuo | PEG | SL | Microfluidic device | 60 |
2011 | Miller | Inorganic–organic hybrid materials | SL | Transdermal bio sensor | 61 |
2019 | Narayanan | Au NPs/W/colloidal Pt | SL | Electrochemical bio sensor | 62 |
2020 | Marzo | PLA/G | FDM | Enzymatic biosensor | 52 |
2020 | Cardosoa | PLA/G | FDM | Electrodes | 53 |
2021 | Kwon | Cu nanoparticles/polyethylene naphthalate | SLS | Flexible touch panel applications | 66 |
Fig. 4 Schematic illustration of the bio-printing process in tissue engineering applications (created with BioRender). |
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