Oncotarget: MicroRNA (miR) dysregulation during Helicobacter pylori-induced gastric



Oncotarget


Volume 11, Issue 10

reported that dysregulation of noncoding micro RNA molecules has been associated with immune cell activation in the context of Helicobacter pylori-induced gastric inflammation as well as carcinogenesis, but also with downregulation of mismatch repair genes, and may interfere with immune checkpoint proteins that lead to the overexpression of antigens on gastric tumor cells.

Among the many micro RNAs involved in gastric inflammation, adenocarcinoma development and immune checkpoint regulation, mi R-155 is notable in that its upregulation is considered a key marker of chronic gastric inflammation that predisposes a patient to gastric carcinogenesis.


Dr. Christian Prinz

from

the Lehrstuhl für Innere Medizin1, University of Witten gGmbH, Helios Universitätsklinikum

said, ”

Increasing evidence suggests that microRNA (miRNA) dysregulation has critical impacts on development, as well as inflammation and cancer development

“Increasing evidence suggests that microRNA (miRNA) dysregulation has critical impacts on development, as well as inflammation and cancer development”

– Dr. Christian Prinz, Lehrstuhl für Innere Medizin1, University of Witten gGmbH, Helios Universitätsklinikum

Notably, it seems that human

gastrointestinal cancer

can be better classified using mi RNA expression profiles than mRNA or protein expression profiles.

Using a new bead-based flow cytometric mi RNA expression profiling method, they performed a systematic expression analysis of 217 mammalian mi RNAs from 334 samples, including multiple human cancers.

Furthermore, they successfully identified poorly differentiated tumors based on mi RNA expression profiles, whereas the classification of the same samples using messenger RNA profiles was highly inaccurate.

Many mi RNAs exhibit differential regulation in cancer, for example, mi R-34a is involved in p53-mediated apoptosis in pancreatic cancer, and nine mi RNAs are upregulated in primary

breast cancer

, including mi R-21, mi R-181b, and mi R-155.

The Prinz Research Team concluded in their

Oncotarget Research Perspective

, ”

clinical strategies aiming to prevent miR-155 overexpression (i. e., via silencer RNAs) may thus represent a promising method of controlling cancer growth (e. g., by allowing DNA repair), especially in

pre-malignant lesions

or during the early stages of gastric cancer.

###


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DOI



https:/

/

doi.

org/

10.

18632/

oncotarget.

27520


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Correspondence to

– Christian Prinz –

[email protected]


Keywords




Helicobacter pylori

,

gastric inflammation

,

gastric cancer

,

microRNA

,

miR-155



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This part of information is sourced from https://www.eurekalert.org/pub_releases/2020-03/ijl-om031320.php

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