Abstract
The liver plays a pivotal role in the clearance of drugs. Reliable assays for liver function are crucial for various metabolism investigation, including toxicity, disease, and pre-clinical testing for drug development. Bile is an aqueous secretion of a functioning liver. Analyses of bile are used to explain drug clearance and related effects and are thus important for toxicology and pharmacokinetic research. Bile fluids collection is extensively performed in vivo, whereas this process is rarely reproduced as in the in vitro studies. The key to success is the technology involved, which needs to satisfy multiple criteria. To ensure the accuracy of subsequent chemical analyses, certain amounts of bile are needed. Additionally, non-invasive and continuous collections are preferable in view of cell culture. In this review, we summarize recent progress and limitations in the field. We highlight attempts to develop advanced liver cultures for bile fluids collection, including methods to stimulate the secretion of bile in vitro. With these strategies, researchers have used a variety of cell sources, extracellular matrix proteins, and growth factors to investigate different cell-culture environments, including three-dimensional spheroids, cocultures, and microfluidic devices. Effective combinations of expertise and technology have the potential to overcome these obstacles to achieve reliable in vitro bile assay systems.
Highlights
The liver is one of the largest glands in the body and is pivotal to various metabolic functions, including blood glucose regulation, protein synthesis, and detoxification
bile acids (BAs) are often used as an index for this purpose and are found in blood samples collected from test subjects
The amount of fluids collected from the culture medium is suggestively low, as presented by BA concentrations in the bile at
Summary
The liver is one of the largest glands in the body and is pivotal to various metabolic functions, including blood glucose regulation, protein synthesis, and detoxification. These functions are mainly performed within the hepatocyte parenchymal cells. The in vitro liver model offers time efficient results and is flexible for human tissues (Soldatow et al, 2013) It is simple, controllable (Xu et al, 2014), allows for intensive analyses (Fatehullah et al, 2016), and exhibits accurate dose–response relationships related to drug analyses (Soldatow et al, 2013). We discuss the current research that both directly and indirectly addresses liver-functional bile production in vitro
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