Soluble suppression of tumorigenicity 2 (sST2) as a predictor of adverse outcomes of chronic heart failure

Andrey Ya. Kravchenko; Кравченко Андрей Яковлевич; Andrey V. Budnevsky; Будневский Андрей Валериевич; Tatiana A. Chernik; Черник Татьяна Александровна; Roman E. Tokmachev; Токмачев Роман Евгеньевич

doi:10.18565/therapy.2023.1.63–69

Soluble suppression of tumorigenicity 2 (sST2) as a predictor of adverse outcomes of chronic heart failure

Authors: Kravchenko A.Y.¹, Budnevsky A.V.¹, Chernik T.A.¹, Tokmachev R.E.¹
Affiliations:
1. N.N. Burdenko Voronezh State Medical University of the Ministry of Healthcare of Russia
Issue: Vol 9, No 1 (2023)
Pages: 63-69
Section: ORIGINAL STUDIES
URL: https://journals.eco-vector.com/2412-4036/article/view/321975
DOI: https://doi.org/10.18565/therapy.2023.1.63–69
ID: 321975

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Abstract
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Abstract

NT-proBNP, which is considered a reference biomarker for the diagnosis and control of chronic heart failure (CHF), has a number of limitations and disadvantages in its use, which makes it relevant to search for other biomarkers that characterize various links in the pathogenesis of CHF.

Purpose of the study: to evaluate the possibilities of soluble tumorigenicity suppressor 2 (sST2) using as a predictor of an adverse outcomes of CHF.

Material and methods. The study included 120 stable CHF patients. There were 37,5% of men (n=45) and 62,5% of women (n=75). The mean age was 66,37±8,47 years. At the first stage of the study, complaints and anamnesis were collected. A physical examination, a complete blood count, a biochemical blood test, an enzyme immunoassay with the determination of NT-proBNP, sST2, hs-CRP and TSH and an echocardiography were also performed. At the second stage, which was organized after 12 months, data were collected on the clinical course and outcomes of CHF.

Results. The median level of sST2 in the study sample was 32,15 ng/ml [22,39; 38,59]. In the group of patients of I FC CHF this indicator was 24,72 ng/ml [17,9; 34,38], in II FC – 28,62 ng/ml [20,84; 36,24], in III FC – 37,11 ng/ml [31,2; 45,59], in FC IV – 37,74 ng/ml [32,14; 46,89]. An increase in the proportion of patients with an adverse outcomes was shown with an elevation in sST2 levels, which also corresponded to an increase in CHF FC.

Conclusion. The data obtained confirm the possibilities of sST2 in predicting the course of CHF. This may allow assessing the risks of an unfavorable course and the effectiveness of the applied treatment in this group of patients.

Keywords

chronic heart failure, soluble suppression of tumorigenicity 2 sST2, prognosis of chronic heart failure

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About the authors

Andrey Ya. Kravchenko

N.N. Burdenko Voronezh State Medical University of the Ministry of Healthcare of Russia

Author for correspondence.
Email: a.kravchenko@vrngmu.ru
ORCID iD: 0000-0003-0297-1735

MD, professor of the Department of faculty therapy

Russian Federation, 394036, Voronezh, 10 Studencheskaya Str.

Andrey V. Budnevsky

N.N. Burdenko Voronezh State Medical University of the Ministry of Healthcare of Russia

Email: avbudnevski@vrngmu.ru
ORCID iD: 0000-0002-1171-2746

MD, professor, head of the Department of faculty therapy

Russian Federation, 394036, Voronezh, 10 Studencheskaya Str.

Tatiana A. Chernik

N.N. Burdenko Voronezh State Medical University of the Ministry of Healthcare of Russia

Email: ch01@mail.ru
ORCID iD: 0000-0003-1371-0848

postgraduate student of the Department of faculty therapy

Russian Federation, 394036, Voronezh, 10 Studencheskaya Str.

Roman E. Tokmachev

N.N. Burdenko Voronezh State Medical University of the Ministry of Healthcare of Russia

Email: r.e.tokmachev@vrngmu.ru
ORCID iD: 0000-0001-6379-4635

PhD of Medical Sciences, associate professor of the Department of faculty therapy

Russian Federation, 394036, Voronezh, 10 Studencheskaya Str.

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