Atherosclerosis may starts early in life and each artery has peculiar characteristics likely affecting atherogenesis. The primary objective of the work was to underpin the microRNA (miR)-profiling differences in human normal femoral, abdominal aortic, and carotid arteries. The secondary aim was to investigate if those identified miRs, differently expressed in normal conditions, may also have a role in atherosclerotic arteries at adult ages. MiR-profiles were performed on normal tissues, revealing that aorta and carotid arteries are more similar than femoral arteries. MiRs emerging from profiling comparisons, i.e., miR-155-5p, -27a-5p, and -139-5p, were subjected to validation by RT-qPCR in normal arteries and also in pathological/atheroma counterparts, considering all the available 20 artery specimens. The three miRs were confirmed to be differentially expressed in normal femoral vs aorta/carotid arteries. Differential expression of those miRs was also observed in atherosclerotic arteries, together with some miR-target proteins, such as vimentin, CD44, E-cadherin and an additional marker SLUG. The different expression of miRs and targets/markers suggests that aorta/carotid and femoral arteries differently activate molecular drivers of pathological condition, thus conditioning the morphology of atheroma in adult life and likely suggesting the future use of artery-specific treatment to counteract atherosclerosis.

MicroRNA profiles of human peripheral arteries and abdominal aorta in normal conditions: MicroRNAs-27a-5p, -139-5p and -155-5p emerge and in atheroma too / Collura S.; Ciavarella C.; Morsiani C.; Motta I.; Valente S.; Gallitto E.; Abualhin M.; Pini R.; Vasuri F.; Franceschi C.; Capri M.; Gargiulo M.; Pasquinelli G.. - In: MECHANISMS OF AGEING AND DEVELOPMENT. - ISSN 0047-6374. - STAMPA. - 198:(2021), pp. 111547.1-111547.8. [10.1016/j.mad.2021.111547]

MicroRNA profiles of human peripheral arteries and abdominal aorta in normal conditions: MicroRNAs-27a-5p, -139-5p and -155-5p emerge and in atheroma too

Collura S.;Ciavarella C.;Morsiani C.;Motta I.;Valente S.;Gallitto E.;Abualhin M.;Pini R.;Vasuri F.;Franceschi C.;Capri M.;Gargiulo M.;Pasquinelli G.
2021

Abstract

Atherosclerosis may starts early in life and each artery has peculiar characteristics likely affecting atherogenesis. The primary objective of the work was to underpin the microRNA (miR)-profiling differences in human normal femoral, abdominal aortic, and carotid arteries. The secondary aim was to investigate if those identified miRs, differently expressed in normal conditions, may also have a role in atherosclerotic arteries at adult ages. MiR-profiles were performed on normal tissues, revealing that aorta and carotid arteries are more similar than femoral arteries. MiRs emerging from profiling comparisons, i.e., miR-155-5p, -27a-5p, and -139-5p, were subjected to validation by RT-qPCR in normal arteries and also in pathological/atheroma counterparts, considering all the available 20 artery specimens. The three miRs were confirmed to be differentially expressed in normal femoral vs aorta/carotid arteries. Differential expression of those miRs was also observed in atherosclerotic arteries, together with some miR-target proteins, such as vimentin, CD44, E-cadherin and an additional marker SLUG. The different expression of miRs and targets/markers suggests that aorta/carotid and femoral arteries differently activate molecular drivers of pathological condition, thus conditioning the morphology of atheroma in adult life and likely suggesting the future use of artery-specific treatment to counteract atherosclerosis.
2021
MicroRNA profiles of human peripheral arteries and abdominal aorta in normal conditions: MicroRNAs-27a-5p, -139-5p and -155-5p emerge and in atheroma too / Collura S.; Ciavarella C.; Morsiani C.; Motta I.; Valente S.; Gallitto E.; Abualhin M.; Pini R.; Vasuri F.; Franceschi C.; Capri M.; Gargiulo M.; Pasquinelli G.. - In: MECHANISMS OF AGEING AND DEVELOPMENT. - ISSN 0047-6374. - STAMPA. - 198:(2021), pp. 111547.1-111547.8. [10.1016/j.mad.2021.111547]
Collura S.; Ciavarella C.; Morsiani C.; Motta I.; Valente S.; Gallitto E.; Abualhin M.; Pini R.; Vasuri F.; Franceschi C.; Capri M.; Gargiulo M.; Pasquinelli G.
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11585/831852
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