Value of Resistin in Early Onset Neonatal Sepsis

Özdemir, Abdurrahman Avar; Elgörmüş, Yusuf

doi:10.1055/s-0037-1608713

Cited by 3 publications

(2 citation statements)

References 28 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Some studies on adult and neonatal patients have reported elevated serum levels during inflammation and infection. The few studies conducted on newborns have suggested that this marker could be an indicator of EOS, but its diagnostic value proved to be less than that of CRP and the cut-off value could not be established with accuracy due to several factors such as control group and number of days since the first sign of sepsis [ 125 , 126 ]. Some biomarkers such as sTREM-1 (human triggering receptor expressed on myeloid cells-1), pentraxin-3 and pro-adrenomedullin, which were found to have high values in infected adults and children, failed to prove their role in neonatal EOS [ 127 ].…”

Section: Biomarkers Commonly Used or Under Consideration For Eos Dmentioning

confidence: 99%

Relevance of Biomarkers Currently in Use or Research for Practical Diagnosis Approach of Neonatal Early-Onset Sepsis

et al. 2020

View full text Add to dashboard Cite

Neonatal early-onset sepsis (EOS) is defined as an invasive infection that occurs in the first 72 h of life. The incidence of EOS varies from 0.5–2% live births in developed countries, up to 9.8% live births in low resource settings, generating a high mortality rate, especially in extremely low birth weight neonates. Clinical signs are nonspecific, leading to a late diagnosis and high mortality. Currently, there are several markers used for sepsis evaluation, such as hematological indices, acute phase reactants, cytokines, which by themselves do not show acceptable sensitivity and specificity for the diagnosis of EOS in neonates. Newer and more selective markers have surfaced recently, such as presepsin and endocan, but they are currently only in the experimental research stages. This comprehensive review article is based on the role of biomarkers currently in use or in the research phase from a basic, translational, and clinical viewpoint that helps us to improve the quality of neonatal early-onset sepsis diagnosis and management.

show abstract

Section: Biomarkers Commonly Used or Under Consideration For Eos Dmentioning

confidence: 99%

Relevance of Biomarkers Currently in Use or Research for Practical Diagnosis Approach of Neonatal Early-Onset Sepsis

et al. 2020

View full text Add to dashboard Cite

show abstract

“…При активации эндотелиальных клеток цитокинами наблюдается быстрое повышение (в течение 1-6 ч) уровня sICAM-1 в сыворотке крови, что делает его маркером системного воспаления. В нас тоящее время существуют разногласия относительно полезности этого маркера для диагностики EOS, поскольку некоторые авторы предложили sICAM-1 в качестве ценного маркера только в первые 4 дня жизни, а другие отметили аналогичные или даже более высокие уровни у здоровых новорожденных в первые 5 дней [40,41]; 5) програнулин -аутокринный фактор роста из 593 аминокислот, который регулирует сигнальную систему TNF/TNFR, может предсказывать сепсис и СПОН у новорожденных > 34 недель беременности [42]; 6) неоптерин -биохимический маркер иммунной активности, повышение которого определяется при клеточно-опосредованном иммунном ответе; 7) резистин (FIZZ3) -белок, богатый цистеином, который играет спорную физиологическую роль в ожирении и инсулинорезистентности и повышается при системном воспалительном ответе у новорожденных, детей и взрослых, однако его диагностическую ценность еще предстоит узнать [43,44]; 8) пресепсин (ПСП) -это белок, являющийся N-концевым фрагментом рецептора макрофагов CD14 [45]. Механизм образования ПСП связан с бактериальным фагоцитозом и расщеплением CD14 лизосомальными ферментами.…”

Section: биомаркеры системного воспаленияunclassified

Multiple organ dysfunction syndrome prediction in newborn children

Golomidov¹,

Grigoryev

Мозес

et al. 2022

Innovacionnaâ medicina Kubani

View full text Add to dashboard Cite

There are several directions for predicting multiple organ dysfunction syndrome (MODS), but almost all of them are poorly tested in neonatology. This review is presented to indicate the problem of the condition severity objectification of newborns and the possibility of predicting the development of MODS. Scales for assessing the severity of MODS in critically ill children have been developed and used since the end of the last century, but their validation in the newborns faces certain difficulties. Prognostic nosospecific scales: NICHD (National Institute of Child Health and Human Development) calculator, CRIB II (Clinical Risk Index for Babies), SNAPPE-II (Score for Neonatal Acute Physiology with Perinatal Extension II) are used in neonatology, however their comparison in this category of patients has not been carried out.Theoretical and practical issues of the short-term and long-term prediction of the MODS onset and its outcomes in newborns is a promising area of neonatology, since it allows a doctor to be warned about an impending catastrophe and opens a “window of opportunity” for timely correction of treatment tactics and complications prevention. Obtaining different phenotypes of critical illness and predicting their outcomes in children may have good predictive potential, but such studies have not been conducted in newborns. A promising direction in predicting MODS is the identification of biomarkers of inflammation, among which endocan, cluster of differentiation 64, cluster of differentiation molecules 11b, “pancreatic stone protein” (PSP), soluble intercellular adhesionmolecule-1 (sICAM-1), progranulin, neopterin, resistin (FIZZ3, presepsin (PSP)) carry a good potential, but their effectiveness in neonatology is still to be investigated.Thus, the prediction of MODS in children and newborns remains an unresolved problem. At the same time, several promising scientific directions are actively being developed today, which may lead to a significant breakthrough in predicting MODS in neonatology.

show abstract

Pathogenesis, Prognosis and Outcomes of Multiple Organ Failure in Newborns (Review)

Golomidov¹,

Grigoriev

Moses

et al. 2022

Obŝaâ reanimatologiâ

View full text Add to dashboard Cite

Multiple organ failure (MOF) is the leading cause of neonatal mortality in intensive care units. The prevalence of MOF in newborns is currently unclear, since its incidence varies in asphyxia, sepsis, prematurity, and comorbidity, and depends on the level of development and funding of health care in different countries. Sepsis and acute respiratory distress syndrome prevail among the causes of MOF in this category of patients.Aim of the review. To summarize the available literature data on the pathogenesis, therapeutic strategies and outcomes of MOF in newborns.Material and methods. We searched PubMed, Scopus, Web of Science, and RSCI databases using the following keywords: «newborns, multiple organ failure, etiology, pathogenesis, premature, diagnosis, treatment, respiratory support, cardiotonic support», without language limitations. A total of 144 full-text sources were selected for analysis, 70% of which were published in the last five years and 50% were published in the last three years. Criteria for exclusion were low information value and outdated data.Results. The prevalence of MOF in neonates is currently unclear. This could be due to common association of neonatal MOF (as well as the adult one) with various diseases; thus, its incidence is not the same for asphyxia, sepsis, prematurity, and comorbidities. There is no precise data on neonatal mortality in MOF, but according to some reports, it may be as high as 13-50%.In newborns, MOF can be caused by two major causes, intrapartum/postnatal asphyxia and sepsis, but could also be influenced by other intranatal factors such as intrauterine infections and acute interruption of placental blood flow.The key element in the pathogenesis of neonate MOF is cytokinemia, which triggers universal critical pathways. Attempts to identify different clinical trajectories of critical illness in various categories of patients have led to the discovery of MOF phenotypes with specific patterns of systemic inflammatory response. This scientific trend is very promising for the creation of new classes of drugs and individual therapeutic pathways in neonates with MOF of various etiologies.The pSOFA scale is used to predict the outcome of neonatal MOF, however, the nSOFA scale has higher validity in premature infants with low birth weight.Central nervous system damage is the major MOF-associated adverse outcome in newborns, with gestational age and the timing of treatment initiation being key factors affecting risk of MOF development in both full-term and premature infants.Conclusion. The study of cellular messengers of inflammation, MOF phenotypes, mitochondrial insufficiency, and immunity in critically ill infants with MOF of various etiologies is a promising area of research. The pSOFA scale is suggested for predicting the outcome of MOF in full-term infants, while the nSOFA scale should be used in premature infants with low birth weight.

show abstract

Value of Resistin in Early Onset Neonatal Sepsis

Cited by 3 publications

References 28 publications

Relevance of Biomarkers Currently in Use or Research for Practical Diagnosis Approach of Neonatal Early-Onset Sepsis

Relevance of Biomarkers Currently in Use or Research for Practical Diagnosis Approach of Neonatal Early-Onset Sepsis

Multiple organ dysfunction syndrome prediction in newborn children

Pathogenesis, Prognosis and Outcomes of Multiple Organ Failure in Newborns (Review)

Contact Info

Product

Resources

About