Expansion of airway basal epithelial cells from primary human non‐small cell lung cancer tumors

Hynds, Robert E.; Aissa, Assma Ben; Gowers, Khc; Tbk, Watkins; Bosshard‐Carter, Leticia; Aj, Rowan; Veeriah, Selvaraju; Wilson, George D.; Quezada, Sergio A.; Swanton, Charles; Janes, Sam M.

doi:10.1002/ijc.31383

Cited by 18 publications

(20 citation statements)

References 27 publications

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“…The irradiated J2 cells can directly serve as feeders. Other way is to use the anti-proliferative mitomycin C (2–4 μg/mL) to treat J2 cells for 1–3 h to acquire feeder cells 25 . However, it is necessary to wash the mitomycin C-treated cells for several times to avoid growth inhibition by mitomycin C during co-cultures.…”

Section: An Overview Of Cr Technologymentioning

confidence: 99%

“…The eligibility of CR to immortalize a wide range of epithelial cells of varied origins has been proved by many researches. Primary cells from both normal and pathological tissues can be proliferated under CR conditions ( Table 2 12 , 25 , 69 , 83 , 100 , 101 , 102 , 103 , 104 , 105 , 106 , 107 , 108 , 109 , 110 , 111 , 112 , 113 , 114 , 115 , 116 , 117 , 118 , 119 , 120 , 121 , 122 , 123 , 124 , 125 , 126 , 127 , 128 , 129 , 130 , 131 , 132 , 133 , 134 , 135 , 136 , 137 , 138 , 139 , 140 , 141 , 142 , 143 , 144 , 145 ). Of particular note, not only human tissues but also tissues from other origins such as mouse, horse, dog and fish have been used for CR culture.…”

Section: Cr Applicationsmentioning

confidence: 99%

“…In the study of Hynds et al. 25 , CR condition only enabled tumor cell culture from 1 out of 10 primary NSCLC tumors. They suggested that expanded CR tumor cells was seen at passage 2, which was rapidly outgrown by normal epithelial cells in later passages 25 .…”

Section: Challengesmentioning

confidence: 99%

“… 25 , CR condition only enabled tumor cell culture from 1 out of 10 primary NSCLC tumors. They suggested that expanded CR tumor cells was seen at passage 2, which was rapidly outgrown by normal epithelial cells in later passages 25 . Notably, this CR tumor cells could form a tumor in NSG mice and re-culture of cells from the tumor xenograft maintained key characteristics of primary tumor 25 .…”

Section: Challengesmentioning

confidence: 99%

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Conditional reprogramming: next generation cell culture

Wang

et al. 2020

Acta Pharmaceutica Sinica B

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Long-term primary culture of mammalian cells has been always difficult due to unavoidable senescence. Conventional methods for generating immortalized cell lines usually require manipulation of genome which leads to change of important biological and genetic characteristics. Recently, conditional reprogramming (CR) emerges as a novel next generation tool for long-term culture of primary epithelium cells derived from almost all origins without alteration of genetic background of primary cells. CR co-cultures primary cells with inactivated mouse 3T3-J2 fibroblasts in the presence of RHO-related protein kinase (ROCK) inhibitor Y-27632, enabling primary cells to acquire stem-like characteristics while retain their ability to fully differentiate. With only a few years’ development, CR shows broad prospects in applications in varied areas including disease modeling, regenerative medicine, drug evaluation, drug discovery as well as precision medicine. This review is thus to comprehensively summarize and assess current progress in understanding mechanism of CR and its wide applications, highlighting the value of CR in both basic and translational researches and discussing the challenges faced with CR.

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Section: An Overview Of Cr Technologymentioning

confidence: 99%

Section: Cr Applicationsmentioning

confidence: 99%

Section: Challengesmentioning

confidence: 99%

Section: Challengesmentioning

confidence: 99%

See 2 more Smart Citations

Conditional reprogramming: next generation cell culture

Wang

et al. 2020

Acta Pharmaceutica Sinica B

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“…The first attempt to solve the disadvantage of cell line "purity" as well as personalization of the treatment approach was the introduction of primary ex vivo cancer cell lines into the cancer research, including drug testing, discovery and therapy response prediction, with improving methodologies and optimizations for cell culturing [175][176][177][178]. Heterogeneity found in cell cultures was suggested to be coded by biological mechanisms from the primary tumors, and it was acknowledged as an instrument for clinical implications.…”

Section: D In Vitro Modelsmentioning

confidence: 99%

Recent Approaches Encompassing the Phenotypic Cell Heterogeneity for Anticancer Drug Efficacy Evaluation

Stulpinas¹,

Imbrasaitė²,

Krestnikova³

et al. 2020

Tumor Progression and Metastasis

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Despite the advancements in biomarker-based personalized cancer therapy, the inadequacy of molecular and genetic profiling in identifying effective drug combinations was defined in most cases. Drug resistance remains a major limitation of the current predictive oncology. Emerging reports indicate that the success of anticancer therapy is usually limited by intratumoral heterogeneity which is not captured by the existing cancer cell biomarker-based approaches. Cell heterogeneity, not only genetic but also phenotypic, is considered to be the root cause of resistance to anticancer treatment, cancer progression, and the presence of cancer stem cells. Therefore, functional testing of live cells representing various cell types within the tumor exposed to potential therapies is needed for identification of effective drug combinations. Here we look at the different existing model systems, including ex vivo models of the patient's tumor cells, 2D/3D in vitro cultures/cocultures, patient-derived cellular organoids, single-cell models, ex vivo tumor platforms containing tumor microenvironment and extracellular matrix, etc., scoping at drug efficacy evaluation and solving the problem of cancer resistance.

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A comprehensive review of 3D cancer models for drug screening and translational research

Sharma,

Dey,

Karmakar

et al. 2023

Cancer Innovation

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The 3D cancer models fill the discovery gap of 2D cancer models and play an important role in cancer research. In addition to cancer cells, a range of other factors include the stroma, density and composition of extracellular matrix, cancer‐associated immune cells (e.g., cancer‐associated fibroblasts cancer cell‐stroma interactions and subsequent interactions, and a number of other factors (e.g., tumor vasculature and tumor‐like microenvironment in vivo) has been widely ignored in the 2D concept of culture. Despite this knowledge, the continued use of monolayer cell culture methods has led to the failure of a series of clinical trials. This review discusses the immense importance of tumor microenvironment (TME) recapitulation in cancer research, prioritizing the individual roles of TME elements in cancer histopathology. The TME provided by the 3D model fulfills the requirements of in vivo spatiotemporal arrangement, components, and is helpful in analyzing various different aspects of drug sensitivity in preclinical and clinical trials, some of which are discussed here. Furthermore, it discusses models for the co‐assembly of different TME elements in vitro and focuses on their synergistic function and responsiveness as tumors. Furthermore, this review broadly describes of a handful of recently developed 3D models whose main focus is limited to drug development and their screening and/or the impact of this approach in preclinical and translational research.

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Expansion of airway basal epithelial cells from primary human non‐small cell lung cancer tumors

Cited by 18 publications

References 27 publications

Conditional reprogramming: next generation cell culture

Conditional reprogramming: next generation cell culture

Recent Approaches Encompassing the Phenotypic Cell Heterogeneity for Anticancer Drug Efficacy Evaluation

A comprehensive review of 3D cancer models for drug screening and translational research

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