Clinical assessment of neutrophil gelatinase-associated lipocalin as a potential diagnostic marker for neonatal sepsis: a prospective cohort study

Midan, Dina A; El-Gendy, Fady M; ELAlla, Dalia Abo; Kotb, Mayada

doi:10.1080/07853890.2022.2091789

Cited by 6 publications

(7 citation statements)

References 27 publications

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“…For diagnosing sepsis, LCN2 was proved to be a sensitive and speci c biomarker to distinguish sepsis from healthy control. At the 475.00 pg/ml cut-off value, LCN2 showed both sensitivity and speci city of 100% with an AUC of 100% to identify sepsis from healthy neonates 37 . While in pediatric sepsis, the AUC was 0.84 at the 125 ng/ml cut-off value, and sensitivity and speci city were 0.813 and 0.806, respectively 38 .…”

Section: Discussionmentioning

confidence: 97%

Plasma exosomes proteome profiling discovers protein markers to identify sepsis

Gong,

Liu,

et al. 2024

Preprint

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Sepsis, a life-threatening clinical issue caused by infection, can be diagnosed early through the analysis of exosomes in plasma. Plasma exosomes were extracted and identified by group (a sepsis group, a non-sepsis group, and a healthy control group). iTRAQ was used to identify the differentially expressed proteins among the three groups. The identified proteins were measured by ELISA in plasma samples. LCN2 and MGP were differentially expressed among the three groups. The median level of LCN2 were 131.93 (96.26,183.65), 52.79 (31.39,89.05) and 33.80 (26.80,47.06) ng/ml in the sepsis, non-sepsis and healthy control group, respectively. The plasma MGP levels in these three groups were 1.16 (1.06,1.30), 0.99 (0.91,1.07) and 0.89 (0.80,1.02) ng/ml, respectively. For both biomarkers, the sepsis group had higher levels than the non-sepsis group(P < 0.05). The area under the curve values of LCN2 and MGP were 0.903 and 0.813, respectively. When combined, these two biomarkers had a sensitivity of 0.900 and a specificity of 0.900 in distinguishing sepsis from non-sepsis. Plasma exosome proteome analysis has revealed that LCN2 and MGP may serve as effective biomarkers for diagnosing sepsis, further research is necessary to validate their diagnostic efficiency.

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Section: Discussionmentioning

confidence: 97%

Plasma exosomes proteome profiling discovers protein markers to identify sepsis

Gong,

Liu,

et al. 2024

Preprint

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“…Таким образом, NGAL можно рассматривать как многообещающий биомаркер для выявления неонатального сепсиса. Уровень NGAL был высоким у умерших от сепсиса новорожденных [9]. В группе больных сепсисом выявлен статистически значимо более высокий уровень NGAL, чем в контрольной группе (1428 против 239.17 пг/мл).…”

Section: липокалин ассоциированный с желатиназой нейтрофиловunclassified

“…В этом случае проблема ранней диагностики практически не решена, что связано с нетипичными клиническими проявлениями неонатального сепсиса [8] и длительностью получения результатов анализа крови на сепсис -посева на стерильность. Таким образом, задача идентификации биомаркеров для ранней диагностики неонатального сепсиса стоит очень остро [9].…”

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Биологические Маркеры Сепсиса

Радыгина,

Мочалова

2023

Microbiology Independent Research Journal (MIR Journal)

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В настоящее время проблема ранней диагностики сепсиса, оценки эффективности проводимой терапии и прогноза течения заболевания крайне актуальна. При сепсисе своевременное оказание медицинской помощи осложнено нечеткостью симптомов и отсутствием специфического диагностического теста. В связи с этим во всем мире ведется поиск биологических маркеров сепсиса: диагностических, прогностических и терапевтических. В обзоре суммированы результаты исследований по диагностической ценности биологических маркеров сепсиса, их чувствительности, специфичности и прогностической ценности из научных публикаций, представленных в международных базах данных.

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“…In this case, the problem of early diagnosis is practically unresolved, due to atypical clinical manifestations of neonatal sepsis [8] and the time-consuming nature of blood culture analysis for sepsis, namely inoculation for sterility testing. Thus, the identification of biomarkers for the early diagnosis of neonatal sepsis is a pressing issue [9].…”

Section: Introductionmentioning

confidence: 99%

Biological markers of sepsis

Radygina,

Mochalova

2023

Microbiology Independent Research Journal (MIR Journal)

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Currently, the issues of early sepsis diagnosis, assessment of the effectiveness of therapies conducted, and disease prognosis are extremely relevant. In the case of sepsis, timely medical assistance is complicated by the ambiguity of symptoms and the absence of a specific diagnostic test. Therefore, the search for sepsis biomarkers with diagnostic, prognostic, and therapeutic potential is underway in medical centers worldwide. This review summarizes research results regarding the diagnostic values of sepsis biomarkers – their sensitivity, specificity, and prognostic value – as presented in scientific publications indexed in international databases.

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Clinical assessment of neutrophil gelatinase-associated lipocalin as a potential diagnostic marker for neonatal sepsis: a prospective cohort study

Cited by 6 publications

References 27 publications

Plasma exosomes proteome profiling discovers protein markers to identify sepsis

Plasma exosomes proteome profiling discovers protein markers to identify sepsis

Биологические Маркеры Сепсиса

Biological markers of sepsis

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