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ECRG4 expression in normal rat tissues: expression study and literature review

Authors

A. Porzionato
University of Padua, Italy.
M. Rucinski
Poznan University of Medical Sciences, Poland.
V. Macchi
University of Padua, Italy.
G. Sarasin
University of Padua, Italy.
L.K. Malendowicz
Poznan University of Medical Sciences, Poland.
R. De Caro
rdecaro@unipd.it
University of Padua, Italy.
The Esophageal Cancer Related Gene 4 (ECRG4) is a highly conserved tumour suppressor gene encoding various peptides (augurin, CΔ16 augurin, ecilin, argilin, CΔ16 argilin) which can be processed and secreted. In the present work, we examined ECRG4 expression and location in a wide range of rat organs and reviewed the available literature. ECRG4 mRNA was identified in all examined tissues by quantitative PCR (qPCR). ECRG4 immunoreaction was mainly cytoplasmic, and was detected in heart and skeletal muscles, smooth muscle cells showing only weak reactions. In the digestive system, ECRG4 immunostaining was stronger in the esophageal epithelium, bases of gastric glands, hepatocytes and pancreatic acinar epithelium. In the lymphatic system, immunoreactive cells were detectable in the thymus cortex, lymph node medulla and splenic red pulp. In the central and peripheral nervous systems, different neuronal groups showed different reaction intensities. In the endocrine system, ECRG4 immunoreaction was detected in the hypothalamic paraventricular and supraoptic nuclei, hypophysis, thyroid and parathyroid glands, adrenal zona glomerularis and medulla and Leydig cells, as well as in follicular and luteal cells of the ovary. In the literature, ECRG4 has been reported to inhibit cell proliferation and increase apoptosis in various cell types. It is down-regulated, frequently due to hypermethylation, in esophageal, prostate, breast and colon cancers, together with glioma (oncosuppressor function), although it is up-regulated in papillary thyroid cancer (oncogenic role). ECRG4 expression is also higher in non-proliferating cells of the lymphatic system. In conclusion, our identification of ECRG4 in many structures suggests the involvement of ECRG4 in the tumorigenesis of other organs and also the need for further research. In addition, on the basis of the location of ECRG4 in neurons and endocrine cells and the fact that it can be secreted, its role as a neurotransmitter/neuromodulator and endocrine factor must be examined in depth in the future.

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Citations

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Qiang Xu, Xiangjie Zhang, Maolin Hao, Xitong Dang, QianQian Xu, Lukas Cyganek, Ibrahim Akin, Dan Tang, Bin Liao, Xiaobo Zhou, Huan Lan (2024)
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Supporting Agencies

Ministry of Science and Education, Poland (grant IP2011 046671).
A. Porzionato, University of Padua
Department of Molecular Medicine, University of Padova
M. Rucinski, Poznan University of Medical Sciences
Department of Histology and Embryology, Poznan University of Medical Sciences
V. Macchi, University of Padua
Department of Molecular Medicine
G. Sarasin, University of Padua
Department of Molecular Medicine
L.K. Malendowicz, Poznan University of Medical Sciences
Department of Histology and Embryology
R. De Caro, University of Padua

Department of Molecular Medicine

How to Cite

Porzionato, A., Rucinski, M., Macchi, V., Sarasin, G., Malendowicz, L., & De Caro, R. (2015). ECRG4 expression in normal rat tissues: expression study and literature review. European Journal of Histochemistry, 59(2). https://doi.org/10.4081/ejh.2015.2458

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