Characterization of doxycycline-dependent inducible Simian Virus 40 large T antigen immortalized human conjunctival epithelial cell line

Mitani, Akira; Kobayashi, Takeshi; Hayashi, Yasuhito; Matsushita, Natsuki; Matsushita, Sachi; Nakao, Saori; Takahira, Naoko; Shiraishi, Atsushi; Ohashi, Yuichi

doi:10.1371/journal.pone.0222454

Cited by 10 publications

(5 citation statements)

References 28 publications

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“…Replicative senescence is a barrier that cells must overcome to become immortalized [ 23 ]. Telomerase regulates the senescence of cells through telomere maintenance and there is evidence that human epithelial cell lines and brain pericyte cell lines can be immortalized or have their in vitro lifespan extended by the transfer of SV40 large T antigen [ 21 , 24 ]. In this study, we introduced SV40 large T antigen lentivirus into primary human lung pericytes.…”

Section: Discussionmentioning

confidence: 99%

Generation of a new immortalized human lung pericyte cell line: a promising tool for human lung pericyte studies

Goodwin

et al. 2021

Laboratory Investigation

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Pericytes apposed to the capillary endothelium are known to stabilize and promote endothelial integrity. Recent studies indicate that lung pericytes play a prominent role in lung physiology, and they are involved in the development of various lung diseases including lung injury in sepsis, pulmonary fibrosis, asthma, and pulmonary hypertension. Accordingly, human lung pericyte studies are important for understanding the mechanistic basis of lung physiology and pathophysiology; however, human lung pericytes can only be cultured for a few passages and no immortalized human lung pericyte cell line has been established so far. Thus, our study aims to establish an immortalized human lung pericyte cell line. Developed using SV40 large T antigen lentivirus, immortalized pericytes exhibit stable SV40T expression, sustained proliferation and have significantly higher telomerase activity compared to normal human lung pericytes. In addition, these cells retained pericyte characteristics, marked by similar morphology, and expression of pericyte cell surface markers such as PDGFRβ, NG2, CD44, CD146, CD90 and CD73. Furthermore, similar to that of primary pericytes, immortalized pericytes promoted endothelial cell tube formation and responded to different stimuli. Our previous data showed that friend leukemia virus integration 1 (Fli-1), a member of the ETS transcription factor family, is a key regulator that modulates inflammatory responses in mouse lung pericytes. We further demonstrated that Fli-1 regulates inflammatory responses in immortalized human lung pericytes. To summarize, we successfully established an immortalized human lung pericyte cell line, which serves as a promising tool for in vitro pericyte studies to understand human lung pericyte physiology and pathophysiology.

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Section: Discussionmentioning

confidence: 99%

Generation of a new immortalized human lung pericyte cell line: a promising tool for human lung pericyte studies

Goodwin

et al. 2021

Laboratory Investigation

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“…Numerous cell lines are derived directly from tumors, while others are generated from primary cells of normal tissues by disabling cell cycle arrest or senescence genes such as p53, Rb, and p16 [ 137 , 138 ]. This can be achieved through spontaneous mutations, shRNA, gene editing, or the overexpression of Simian Vacuolating Virus 40 large T antigen [ [139] , [140] , [141] , [142] ]. Therefore, cell lines are capable of continuous proliferation, making it easy and cost-effective to produce a large quantity of cells.…”

Section: Cell Sources For 3d Bioprintingmentioning

confidence: 99%

Advancements of 3D bioprinting in regenerative medicine: Exploring cell sources for organ fabrication

Ma,

Deng,

et al. 2024

Heliyon

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“…Recently, Mitani et al developed a 3D model of the conjunctiva containing rabbit primary conjunctival fibroblasts and a new human conjunctival epithelial cell line, called iHCjECs [ 159 ]. They used collagen gels as the scaffold, into which the fibroblasts were embedded.…”

Section: Three-dimensional In Vitro Models Of Anterior Eye Tissuesmentioning

confidence: 99%

Three-Dimensional Human Cell Culture Models to Study the Pathophysiology of the Anterior Eye

García-Posadas

Diebold

2020

Pharmaceutics

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In recent decades, the establishment of complex three-dimensional (3D) models of tissues has allowed researchers to perform high-quality studies and to not only advance knowledge of the physiology of these tissues but also mimic pathological conditions to test novel therapeutic strategies. The main advantage of 3D models is that they recapitulate the spatial architecture of tissues and thereby provide more physiologically relevant information. The eye is an extremely complex organ that comprises a large variety of highly heterogeneous tissues that are divided into two asymmetrical portions: the anterior and posterior segments. The anterior segment consists of the cornea, conjunctiva, iris, ciliary body, sclera, aqueous humor, and the lens. Different diseases in these tissues can have devastating effects. To study these pathologies and develop new treatments, the use of cell culture models is instrumental, and the better the model, the more relevant the results. Thus, the development of sophisticated 3D models of ocular tissues is a significant challenge with enormous potential. In this review, we present a comprehensive overview of the latest advances in the development of 3D in vitro models of the anterior segment of the eye, with a special focus on those that use human primary cells.

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Characterization of doxycycline-dependent inducible Simian Virus 40 large T antigen immortalized human conjunctival epithelial cell line

Cited by 10 publications

References 28 publications

Generation of a new immortalized human lung pericyte cell line: a promising tool for human lung pericyte studies

Generation of a new immortalized human lung pericyte cell line: a promising tool for human lung pericyte studies

Advancements of 3D bioprinting in regenerative medicine: Exploring cell sources for organ fabrication

Three-Dimensional Human Cell Culture Models to Study the Pathophysiology of the Anterior Eye

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