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Adropin as a potential marker of enzyme-positive acute coronary syndrome

AIM: Enzyme-positive acute coronary syndrome (EPACS) can cause injury to or death of the heart muscle owing to prolonged ischaemia. Recent research has indicated that in addition to liver and brain cells, cardiomyocytes also produce adropin. We hypothesised that adropin is released into the bloodstr...

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Autores principales: Aydin, Suna, Eren, Mehmet Nesimi, Yilmaz, Musa, Yardim, Meltem, Aydin, Suleyman, Kalayci, Mehmet, Alatas, Omer Dogan, Kuloglu, Tuncay, Balaban, Heseyin, Cakmak, Tolga, Kobalt, Mehmet Ali, Çelik, Ahmet
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Clinics Cardive Publishing 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5423434/
https://www.ncbi.nlm.nih.gov/pubmed/27196807
http://dx.doi.org/10.5830/CVJA-2016-055
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author Aydin, Suna
Eren, Mehmet Nesimi
Yilmaz, Musa
Yardim, Meltem
Aydin, Suleyman
Kalayci, Mehmet
Alatas, Omer Dogan
Kuloglu, Tuncay
Balaban, Heseyin
Cakmak, Tolga
Kobalt, Mehmet Ali
Çelik, Ahmet
author_facet Aydin, Suna
Eren, Mehmet Nesimi
Yilmaz, Musa
Yardim, Meltem
Aydin, Suleyman
Kalayci, Mehmet
Alatas, Omer Dogan
Kuloglu, Tuncay
Balaban, Heseyin
Cakmak, Tolga
Kobalt, Mehmet Ali
Çelik, Ahmet
author_sort Aydin, Suna
collection PubMed
description AIM: Enzyme-positive acute coronary syndrome (EPACS) can cause injury to or death of the heart muscle owing to prolonged ischaemia. Recent research has indicated that in addition to liver and brain cells, cardiomyocytes also produce adropin. We hypothesised that adropin is released into the bloodstream during myocardial injury caused by acute coronary syndrome (ACS), so serum and saliva levels rise as the myocytes die. Therefore, it could be useful to investigate how ACS affects the timing and significance of adropin release in human subjects METHODS: Samples were taken over three days after admission, from 22 EPACS patients and 24 age- and gendermatched controls. The three major salivary glands (submandibular, sublingual and parotid) were immunohistochemically screened for adropin production, and serum and saliva adropin levels were measured by an enzyme-linked immunosorbent assay (ELISA). Salivary gland cells produce and secrete adropin locally. RESULTS: Serum adropin, troponin I, CK and CK-MB concentrations in the EPACS group became gradually higher than those in the control group up to six hours (p < 0.05), and troponin I continued to rise up to 12 hours after EPACS. The same relative increase in adropin level was observed in the saliva. Troponin I, CK and CK-MB levels started to decrease after 12 hours, while saliva and serum adropin levels started to decrease at six hours after EPACS. In samples taken four hours after EPACS, when the serum adropin value averaged 4.43 ng/ml, the receiver operating characteristic curve showed that the serum adropin concentration indicated EPACS with 91.7% sensitivity and 50% specificity, while when the cut-off adropin value in saliva was 4.12 ng/ml, the saliva adropin concentration indicated EPACS with 91.7% sensitivity and 57% specificity. CONCLUSION: In addition to cardiac troponin and CK-MB assays, measurement of adropin level in saliva and serum samples is a potential marker for diagnosing EPACS.
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spelling pubmed-54234342017-05-24 Adropin as a potential marker of enzyme-positive acute coronary syndrome Aydin, Suna Eren, Mehmet Nesimi Yilmaz, Musa Yardim, Meltem Aydin, Suleyman Kalayci, Mehmet Alatas, Omer Dogan Kuloglu, Tuncay Balaban, Heseyin Cakmak, Tolga Kobalt, Mehmet Ali Çelik, Ahmet Cardiovasc J Afr Cardiovascular Topics AIM: Enzyme-positive acute coronary syndrome (EPACS) can cause injury to or death of the heart muscle owing to prolonged ischaemia. Recent research has indicated that in addition to liver and brain cells, cardiomyocytes also produce adropin. We hypothesised that adropin is released into the bloodstream during myocardial injury caused by acute coronary syndrome (ACS), so serum and saliva levels rise as the myocytes die. Therefore, it could be useful to investigate how ACS affects the timing and significance of adropin release in human subjects METHODS: Samples were taken over three days after admission, from 22 EPACS patients and 24 age- and gendermatched controls. The three major salivary glands (submandibular, sublingual and parotid) were immunohistochemically screened for adropin production, and serum and saliva adropin levels were measured by an enzyme-linked immunosorbent assay (ELISA). Salivary gland cells produce and secrete adropin locally. RESULTS: Serum adropin, troponin I, CK and CK-MB concentrations in the EPACS group became gradually higher than those in the control group up to six hours (p < 0.05), and troponin I continued to rise up to 12 hours after EPACS. The same relative increase in adropin level was observed in the saliva. Troponin I, CK and CK-MB levels started to decrease after 12 hours, while saliva and serum adropin levels started to decrease at six hours after EPACS. In samples taken four hours after EPACS, when the serum adropin value averaged 4.43 ng/ml, the receiver operating characteristic curve showed that the serum adropin concentration indicated EPACS with 91.7% sensitivity and 50% specificity, while when the cut-off adropin value in saliva was 4.12 ng/ml, the saliva adropin concentration indicated EPACS with 91.7% sensitivity and 57% specificity. CONCLUSION: In addition to cardiac troponin and CK-MB assays, measurement of adropin level in saliva and serum samples is a potential marker for diagnosing EPACS. Clinics Cardive Publishing 2017 /pmc/articles/PMC5423434/ /pubmed/27196807 http://dx.doi.org/10.5830/CVJA-2016-055 Text en Copyright © 2015 Clinics Cardive Publishing http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Cardiovascular Topics
Aydin, Suna
Eren, Mehmet Nesimi
Yilmaz, Musa
Yardim, Meltem
Aydin, Suleyman
Kalayci, Mehmet
Alatas, Omer Dogan
Kuloglu, Tuncay
Balaban, Heseyin
Cakmak, Tolga
Kobalt, Mehmet Ali
Çelik, Ahmet
Adropin as a potential marker of enzyme-positive acute coronary syndrome
title Adropin as a potential marker of enzyme-positive acute coronary syndrome
title_full Adropin as a potential marker of enzyme-positive acute coronary syndrome
title_fullStr Adropin as a potential marker of enzyme-positive acute coronary syndrome
title_full_unstemmed Adropin as a potential marker of enzyme-positive acute coronary syndrome
title_short Adropin as a potential marker of enzyme-positive acute coronary syndrome
title_sort adropin as a potential marker of enzyme-positive acute coronary syndrome
topic Cardiovascular Topics
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5423434/
https://www.ncbi.nlm.nih.gov/pubmed/27196807
http://dx.doi.org/10.5830/CVJA-2016-055
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