New Gene Markers for Metabolic Processes and Homeostasis in Porcine Buccal Pouch Mucosa during Cells Long Term-Cultivation-A Primary Culture Approach

Marta Dyszkiewicz-Konwińska; Mariusz J Nawrocki; Yan Huang; Artur Bryja; Piotr Celichowski; Maurycy Jankowski; Katarzyna Błochowiak; Katarzyna Mehr; Małgorzata Bruska; Michał Nowicki; Maciej Zabel; Bartosz Kempisty

doi:10.3390/ijms19041027

New Gene Markers for Metabolic Processes and Homeostasis in Porcine Buccal Pouch Mucosa during Cells Long Term-Cultivation-A Primary Culture Approach

Int J Mol Sci. 2018 Mar 29;19(4):1027. doi: 10.3390/ijms19041027.

Authors

Marta Dyszkiewicz-Konwińska^{1

2}, Mariusz J Nawrocki³, Yan Huang^{4

5}, Artur Bryja⁶, Piotr Celichowski⁷, Maurycy Jankowski⁸, Katarzyna Błochowiak⁹, Katarzyna Mehr¹⁰, Małgorzata Bruska¹¹, Michał Nowicki¹², Maciej Zabel^{13

14}, Bartosz Kempisty^{15

16

17}

Affiliations

¹ Department of Anatomy, Poznań University of Medical Science, 6 Święcickiego St., 60-781 Poznań, Poland. m.dyszkiewicz@ump.edu.pl.
² Department of Biomaterials and Experimental Dentistry, Poznań University of Medical Sciences, 61-701 Poznań, Poland. m.dyszkiewicz@ump.edu.pl.
³ Department of Anatomy, Poznań University of Medical Science, 6 Święcickiego St., 60-781 Poznań, Poland. mjnawrocki@ump.edu.pl.
⁴ OMFS IMPATH Research Group, Department of Imaging & Pathology, Faculty of Medicine, University of Leuven and Oral & Maxillofacial Surgery, University Hospitals Leuven, 3001 Leuven, Belgium. yanhuangcn@gmail.com.
⁵ State Key Laboratory of Oral Diseases, West China College of Stomatology, Sichuan University, 610041 Chengdu, China. yanhuangcn@gmail.com.
⁶ Department of Anatomy, Poznań University of Medical Science, 6 Święcickiego St., 60-781 Poznań, Poland. abryja@ump.edu.pl.
⁷ Department of Histology and Embryology, Poznań University of Medical Science, 6 Święcickiego St., 60-781 Poznań, Poland. pcelichowski@ump.edu.pl.
⁸ Department of Anatomy, Poznań University of Medical Science, 6 Święcickiego St., 60-781 Poznań, Poland. m.jankowski.14@aberdeen.ac.uk.
⁹ Department of Oral Surgery, Poznań University of Medical Sciences, 61-701 Poznań, Poland. kblochowiak@ump.edu.pl.
¹⁰ Department of Oral Rehabilitation, Poznań University of Medical Sciences, 61-701 Poznań, Poland. katarzynamehr@gmail.com.
¹¹ Department of Anatomy, Poznań University of Medical Science, 6 Święcickiego St., 60-781 Poznań, Poland. mbruska@ump.edu.pl.
¹² Department of Histology and Embryology, Poznań University of Medical Science, 6 Święcickiego St., 60-781 Poznań, Poland. mnowicki@ump.edu.pl.
¹³ Department of Histology and Embryology, Poznań University of Medical Science, 6 Święcickiego St., 60-781 Poznań, Poland. mazab@ump.edu.pl.
¹⁴ Department of Histology and Embryology, Wrocław University of Medical Sciences, 50-367 Wrocław, Poland. mazab@ump.edu.pl.
¹⁵ Department of Anatomy, Poznań University of Medical Science, 6 Święcickiego St., 60-781 Poznań, Poland. bkempisty@ump.edu.pl.
¹⁶ Department of Histology and Embryology, Poznań University of Medical Science, 6 Święcickiego St., 60-781 Poznań, Poland. bkempisty@ump.edu.pl.
¹⁷ Department of Obstetrics and Gynecology, University Hospital and Masaryk University, 60177 Brno, Czech Republic. bkempisty@ump.edu.pl.

Abstract

The oral mucosal tissue is a compound structure composed of morphologically and physiologically different cell types. The morphological modification involves genetically determined lifespan, which may be recognized as the balance between cell survival and apoptosis. Although the biochemical processes and pathways in oral mucosa, with special regards to drug transport, delivery, and metabolism, are well known, the cellular physiological homeostasis in this tissue requires further investigation. The porcine buccal pouch mucosal cells (BPMCs) collected from 20 pubertal crossbred Landrace gilts, were used in this study. Immediately after recovery, the oral mucosa was separated micro-surgically, and treated enzymatically. The dispersed cells were transferred into primary in vitro culture systems for a long-term cultivation of 30 days. After each step of in vitro culture (IVC), the cells were collected for isolation of total RNA at 24 h, 7, 15, and 30 days of IVC. While the expression was analyzed for days 7, 15, and 30, the 24th hour was used as a reference for outcome calibration. The gene expression profile was determined using Affymetrix microarray assays and necessary procedures. In results, we observed significant up-regulation of SCARB1, PTGS2, DUSP5, ITGB3, PLK2, CCL2, TGFB1, CCL8, RFC4, LYN, ETS1, REL, LIF, SPP1, and FGER1G genes, belonging to two ontological groups, namely "positive regulation of metabolic process", and "regulation of homeostatic process" at 7 day of IVC as compared to down-regulation at days 15 and 30. These findings suggest that the metabolic processes and homeostatic regulations are much more intense in porcine mucosal cells at day 7 of IVC. Moreover, the increased expression of marker genes, for both of these ontological groups, may suggest the existence of not only "morphological lifespan" during tissue keratinization, but also "physiological checkpoint" dedicated to metabolic processes in oral mucosa. This knowledge may be useful for preclinical experiments with drugs delivery and metabolism in both animals and humans.

Keywords: homeostasis; metabolic process; oral mucosa.

MeSH terms

Animals
Cells, Cultured
Epithelial Cells / cytology
Epithelial Cells / metabolism*
Gene Expression Regulation*
Homeostasis*
Humans
Mouth Mucosa / cytology
Mouth Mucosa / metabolism*
Swine