Evaluation of a panel of 28 biomarkers for the non-invasive diagnosis of endometriosis

Vodolazkaia, Alexandra; El-Aalamat, Y.; Popović, Dušan; Mihályi, Attila; Bossuyt, Xavier; Kyama, Cleophas; Fassbender, Amelie; Bokor, Attila; Schols, Dominique; Huskens, Dana; Meuleman, Christel; Peeraer, Karen; Tomassetti, Carla; Gevaert, Olivier; Waelkens, Etienne; Kasran, Ahmad; Moor, Bart De; D’Hooghe, Thomas

doi:10.1093/humrep/des234

Cited by 162 publications

(189 citation statements)

References 74 publications

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“…Increased serum IL-6 levels observed in patients with minimal-mild endometriosis in our study are in line with findings of some reports [18][19][20] but depart from others that found no value for serum IL-6 in the diagnosis of endometriosis at any stage [21,22] and from yet others that reported slightly elevated serum IL-6 levels in controls [23][24][25]. Additionally, it is worthwhile to note that serum IL-6 was the only marker that was constantly elevated in all our comparison groups (endometriosis group, minimalmild endometriosis group and moderate-severe endometriosis group).…”

Section: Discussionsupporting

confidence: 90%

Experimental immunology Non-invasive diagnosis of endometriosis based on a combined analysis of four plasma biomarkers

Yagmur¹,

Baştu²,

Balcı³

et al. 2013

cejoi

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(46.70 ±27.08 vs. 27.08 ±16.29, p < 0.05; 49.39 ±28.32 vs. 9.78 ±3.87, respectively). In women with minimal-mild endometriosis, only the plasma level of p < 0.05). In women with moderatesevere endometriosis, plasma levels of IL-6 and CA-125 were significantly increased, and those of Epo and tumor necrosis factor α (TNF-α) were significantly decreased (44.53 ±31.07 vs. 27.08 ±16.29, p < 0.05; 57.84 ±61.44 vs. 9.78 ±3.87, p < 0.05; 26.60 ±10.19 vs. 30.32 ±7.94, p < 0.05; 58.61 ±7.93 vs. 65.40 ±9.86, p < 0.05, respectively). The area under curve (AUC) for Epo, 0.322, 0.729 and 0.864, respectively. Conclusions:The results of our study show that progression of endometriosis is associated with the elevated level of serum IL-6. Clearly, larger prospective studies are required to determine the diagnostic potential of measuring circulating inflammatory cytokine levels like IL-6 in endometriosis.

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Section: Discussionsupporting

confidence: 90%

Experimental immunology Non-invasive diagnosis of endometriosis based on a combined analysis of four plasma biomarkers

Yagmur¹,

Baştu²,

Balcı³

et al. 2013

cejoi

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“…18 More recently it was reported that in plasma samples obtained during menstruation, multivariate analysis of 4 biomarkers (annexin V, VEGF, CA-125, and sICAM-1/or glycodelin) enabled the diagnosis of endometriosis undetectable by ultrasound with a sensitivity of 81% to 90% and a specificity of 63% to 81% in independent training and test data sets. 19 Peptide fingerprinting using proteomic analysis of plasma may also have utility as a noninvasive or semi-invasive diagnostic for endometriosis. 20 Taken together, these data suggest that endometriosis biomarkers can be developed using a panel of ''known'' biomarkers or by the discovery of new biomarkers based on proteomic, microarray, metabolomic analysis, or other systems biology approaches.…”

Section: Diagnosismentioning

confidence: 99%

Defining Future Directions for Endometriosis Research: Workshop Report From the 2011 World Congress of Endometriosis in Montpellier, France

D’Hooghe²,

et al. 2013

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Endometriosis, defined as estrogen-dependent lesions containing endometrial glands and stroma outside the uterus, is a chronic and often painful gynecological condition that affects 6% to 10% of reproductive age women. Endometriosis has estimated annual costs of US $12 419 per woman (approximately €9579), comprising one-third of the direct health care costs with two-thirds attributed to loss of productivity. Decreased quality of life is the most important predictor of direct health care and total costs. It has been estimated that there is a mean delay of 6.7 years between onset of symptoms and a surgical diagnosis of endometriosis, and each affected woman loses on average 10.8 hours of work weekly, mainly owing to reduced effectiveness while working. To encourage and facilitate research into this debilitating disease, a consensus workshop to define future directions for endometriosis research was held as part of the 11th World Congress on Endometriosis in September 2011 in Montpellier, France. The objective of this workshop was to review and update the endometriosis research priorities consensus statement developed following the 10th World Congress on Endometriosis in 2008. 1 A total of 56 recommendations for research have been developed, grouped under 6 subheadings: (1) diagnosis, (2) classification and prognosis, (3) clinical trials, treatment, and outcomes, (4) epidemiology, (5) pathophysiology, and (6) research policy. By producing this consensus international research priorities statement, it is the hope of the workshop participants that researchers will be encouraged to develop new interdisciplinary research proposals that will attract increased funding support for work on endometriosis.

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“…Однако ни один биомаркер, ни панель биомар-керов не утверждена в качестве надежного неинва-зивного метода диагностики эндометриоза [29,30]. Возможно, это связано с тем, что большинство ис-следований включали ограниченное число пациен-ток, проводились в различные фазы менструального цикла, не оценивалась стадия заболевания и локали-зация поражений (перитонеальная форма, инфиль-тративный эндометриоз, эндометриоидная киста яичника).…”

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“…[30] про-веден многомерный анализ 28 биомаркеров. Авторы изучали биомаркеры в плазме крови у женщин с хи-рургически подтвержденным диагнозом эндометри-оза и без такового (контрольная группа).…”

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“…Авторы изучали биомаркеры в плазме крови у женщин с хи-рургически подтвержденным диагнозом эндометри-оза и без такового (контрольная группа). В результа-те исследователям удалось разработать две модели, каждая из которых включала 4 биомаркера: модель I (аннексин V, сосудистый эндотелиальный фактор роста (СЭФР), CA-125 и гликоделин) и модель II (аннексин V, СЭФР, CA-125 и растворимые внутри-клеточные адгезивные молекулы-1), характеризую-щихся высокой чувствительностью (81-90%) и специфичностью (63-81%) к эндометриозу, не под-тверждаемому с помощью ультразвукового исследо-вания [30]. Определение вышеназванных показате-лей у пациенток проводилось во время менструации.…”

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The diagnosis of endometriosis with the help of mass spectrometry (a review)

Borisova¹,

Kozachenko²,

Starodubceva³

et al. 2015

Probl. reprod.

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Evaluation of a panel of 28 biomarkers for the non-invasive diagnosis of endometriosis

Cited by 162 publications

References 74 publications

Experimental immunology Non-invasive diagnosis of endometriosis based on a combined analysis of four plasma biomarkers

Experimental immunology Non-invasive diagnosis of endometriosis based on a combined analysis of four plasma biomarkers

Defining Future Directions for Endometriosis Research: Workshop Report From the 2011 World Congress of Endometriosis in Montpellier, France

The diagnosis of endometriosis with the help of mass spectrometry (a review)

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