Arginin-stimulated Copeptin in Polyuria-polydipsia Syndrome in Children
NCT ID: NCT06604975
Last Updated: 2025-02-13
Study Results
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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NOT_YET_RECRUITING
NA
155 participants
INTERVENTIONAL
2025-03-31
2028-07-31
Brief Summary
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The aim of the study is identify the best discriminant threshold of the arginine stimulation test in the uncertain diagnosis (basal copeptin \<30 pmol/l) in the polyuro-polydipsic syndrome in children.
Then evaluate the discriminative capacities of the arginine stimulation test between the primary polydipsia and central insipid diabetes in the polyuro-polydipsic syndrome in children. And finally evaluate the cost-effectiveness of a new decisional algorithm for the differential diagnosis of PPS in children and evaluate the impact of infusion volume on copeptin secretion using the protidemia copeptin ratio.
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Detailed Description
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Patients with basal copeptin value over 3.53 pmol/L are considered as positive diagnosis of PP (Se 100%, Sp 87.4%) and cerebral MRI is not performed for this group of patients (PP group).
Patients with basal copeptin value \< 3.53 pmol/L are considered as an uncertain diagnosis (UD) and cerebral and pituitary MRI is performed with a least two independent interpretations. Abnormal pituitary MRI allows a diagnosis of CDI leading to etiological investigations and AVP treatment. Patients with basal copeptin ≥ 3.53 pmol/l (PP group), and UD patients with normal MRI have gradual reduction of water intake without AVP treatment. For all these latest patients, a clinical and biological reevaluation is performed one month later.
The gold standard will be the final diagnosis PP vs. CDI based on a set of indicators: medical history, physical examination, pituitary hormonal assessment, hypothalamo-pituitary MRI, follow-up at 1 month.
Conditions
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Study Design
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NA
SINGLE_GROUP
DIAGNOSTIC
NONE
Study Groups
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NDI-PP- CDI groups
Copeptin represents a new biomarker, direct mirror of AVP release with remarkable characteristics (stable, rapid determination, small blood volume). Copeptin has become a diagnostic tool in adult PPS and eliminated WDT in the diagnostic process. In children, basal copeptin values help for NDI and to exclude CDI (basal copeptin threshold \> 30 and \>3.53 pmol/l (Se 100%, Sp 87.4%), respectively). Below 3.53 pmol/l, basal copeptin performance was inadequate to discriminate PP and CDI, highlighting the relevance of the stimulated copeptin study to improve this strategy.
Measure of Basal Copeptin level
Copeptin test is performed after solid fasting since midnight without water restriction. After blood collection on heparin tube used for biological inclusion criteria, heparinized plasma is transferred to Timone University hospital (transport temperature +4°C) for screening copeptin assay.
The basal copeptin level determines the next step:
1. copeptin ≥ 30 pmol/L defines the diagnosis of NDI and results in a specific care;
2. copeptin \< 30 pmol/L defines the group of eligible patients for arginine stimulation
Measure of arginine-stimulated copeptin
The arginine-stimulated copeptin test start at 8 am, after solid fasting since midnight without water restriction, and 30 min of rest in decubitus position. A dose of 0.5 g/kg of arginine (maximum 40g) diluted in 0.9% NaCl is infused over 30 min through a peripheral venous line. Copeptin is measured at T0 (before infusion), T45, T60, T90, and T120 min after infusion.
IRM
Based on our previous study, patients with basal copeptin value over 3.53 pmol/L are considered as positive diagnosis of PP (Se 100%, Sp 87.4%) and cerebral MRI is not performed for this group of patients (PP group).
A cerebral and pituitary MRI performed according to reference procedures (without and with contrast medium used in routine care) for patients considered as an uncertain diagnosis (UD) based on basal copeptin value (\&lt; 3.53 pmol/L). MRI interpretation is performed by two independent neuroradiologists (one from the recruiting center and one from the pilot center). In case of discrepancies, a third independent interpretation will be performed by a neuroradiologist from the coordinating center. Abnormal pituitary MRI (thickened pituitary stalk pituitary tumor, ectopic neurohypophysis, septo-optic dysplasia, empty sellar, Rathke pouch) allows a diagnosis of CDI leading to etiological investigations and AVP treatment.
Water reduction at home
Patients with basal copeptin ≥ 3.53 pmol/l (PP group), and UD patients with normal MRI have gradual reduction of water intake at home without AVP treatment : gradual reduction with 20% in the first week, 30% in the second, 40% in the third, reaching 50% of daily fluid in the last week including restriction overnight, deletion drink before sleep. Some recommendations will be provided to help physicians. For all these latest patients, a clinical reassessment (weight, height, heart rate, blood pressure, input/output 24 hours balance) is performed one month later.
Interventions
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Measure of Basal Copeptin level
Copeptin test is performed after solid fasting since midnight without water restriction. After blood collection on heparin tube used for biological inclusion criteria, heparinized plasma is transferred to Timone University hospital (transport temperature +4°C) for screening copeptin assay.
The basal copeptin level determines the next step:
1. copeptin ≥ 30 pmol/L defines the diagnosis of NDI and results in a specific care;
2. copeptin \< 30 pmol/L defines the group of eligible patients for arginine stimulation
Measure of arginine-stimulated copeptin
The arginine-stimulated copeptin test start at 8 am, after solid fasting since midnight without water restriction, and 30 min of rest in decubitus position. A dose of 0.5 g/kg of arginine (maximum 40g) diluted in 0.9% NaCl is infused over 30 min through a peripheral venous line. Copeptin is measured at T0 (before infusion), T45, T60, T90, and T120 min after infusion.
IRM
Based on our previous study, patients with basal copeptin value over 3.53 pmol/L are considered as positive diagnosis of PP (Se 100%, Sp 87.4%) and cerebral MRI is not performed for this group of patients (PP group).
A cerebral and pituitary MRI performed according to reference procedures (without and with contrast medium used in routine care) for patients considered as an uncertain diagnosis (UD) based on basal copeptin value (\&lt; 3.53 pmol/L). MRI interpretation is performed by two independent neuroradiologists (one from the recruiting center and one from the pilot center). In case of discrepancies, a third independent interpretation will be performed by a neuroradiologist from the coordinating center. Abnormal pituitary MRI (thickened pituitary stalk pituitary tumor, ectopic neurohypophysis, septo-optic dysplasia, empty sellar, Rathke pouch) allows a diagnosis of CDI leading to etiological investigations and AVP treatment.
Water reduction at home
Patients with basal copeptin ≥ 3.53 pmol/l (PP group), and UD patients with normal MRI have gradual reduction of water intake at home without AVP treatment : gradual reduction with 20% in the first week, 30% in the second, 40% in the third, reaching 50% of daily fluid in the last week including restriction overnight, deletion drink before sleep. Some recommendations will be provided to help physicians. For all these latest patients, a clinical reassessment (weight, height, heart rate, blood pressure, input/output 24 hours balance) is performed one month later.
Eligibility Criteria
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Inclusion Criteria
* Basal copeptin of less than 30 pmol/l
* Agreeing to participate in the study
* Whose two parents' consent to have their child participate in the study.
Exclusion Criteria
* Unbalanced dysthyroidism
* Corticotropic deficiency
* Ionic disorders (dysnatremia \< 135 or \> 145 mmol/l, dyskalemia \< 3 or \> 5 mmol/l, corrected dyscalcemia \< 2.2 or \> 2.6 mmol/L)
* Moderate to severe clinical dehydration (recent weight loss \> 5% of body weight, clinical or biological signs of dehydration) requiring immediate therapeutic management
* Renal failure with GFR \< 60 mL/min/1.73 m2
* Uropathy
* Tumor syndrome (except hypothalamo-pituitary tumor)
* Intracranial hypertension
* ROHHAD syndrome
* Fever or biological inflammatory syndrome with CRP \> 5 mg/L
* Hepatic insufficiency
* Contraindication to MRI
* Contraindication to progressive water intake restrictions
* History of contraindication to arginine
* Positive test for Pregnancy
* Lack of authorization by both parents or legal representatives
2 Years
18 Years
ALL
No
Sponsors
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Assistance Publique Hopitaux De Marseille
OTHER
Responsible Party
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Principal Investigators
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Rachel REYNAUD, Pr
Role: PRINCIPAL_INVESTIGATOR
AP-HM
Locations
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CHU Angers
Angers, , France
CHU de Bordeaux
Bordeaux, , France
CHU Lille
Lille, , France
HCL
Lyon, , France
Assistance Publique Hopitaux de Marseille
Marseille, , France
CHU Montpellier
Montpellier, , France
CHU Nantes
Nantes, , France
CHU Nice
Nice, , France
AP-HP
Paris, , France
CH Pau
Pau, , France
CHU Reims
Reims, , France
CHU Rennes
Rennes, , France
CHU Rouen
Rouen, , France
CHU Toulouse
Toulouse, , France
Countries
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Central Contacts
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Facility Contacts
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Other Identifiers
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RCAPHM23_0379
Identifier Type: -
Identifier Source: org_study_id
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