International Symposium On The Ehlers-Danlos Syndrome .

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International symposium on the Ehlers-Danlos syndromeGhent (Belgium). September 26-29, 2018CLINICAL DIAGNOSIS OF EHLERS-DANLOS SYNDROME.NEW FUNDAMENTAL INSIGHTS INTO THE CLINICAL SETTING.Hamonet Claude* **, MD, PhD, Manicourt Daniel***, MD, PhD,Hermanns-Lê Trinh****, MD, PhD, Pommeret Stanislas*****, PhD*Department of medicine, University Paris-East-Creteil (UPEC), 8 rue du GénéralSarail 94010 Créteil France.** ELLAsanté, Prevention and Health Center, 29 bis rued'Astorg 75008 Paris. *** Rheumatology Department, Universitary Hospital Saint-Luc,Belgium.****Dermatopathology Department Unilab, Universitary center Liège Belgium.*****Société Chimique de France, Paris.IntroductionIf we trace this disease’s description history through the successive interests ofdermatologists (cutis laxa), rheumatologists (joints hypermobility), geneticists(research of collagens mutations and genetic classification), we better understandwhy such a frequent pathology is never diagnosed or with an average delay ofmore than 20 years after the onset of the first signs.Histogram of the latency time between the first symptoms of the EDS and itsdiagnosis (636 evaluations).During the last decades, studies of the Ehlers-Danlos syndrome have added manysigns/symptoms to the stretchy skin and generalized joints hypermobility making EDSa multifaceted systemic disease (Grahame 1960). This controlled study aimed toidentify the smallest number of additional clinical signs enabling EDS diagnosis withcertainty.Patients and methods.We prospectively assessed 853 EDS patients attending our outpatient ward betweenJune 2014 and June 2017. They all met the 1997 Villefranche criteria. These

patients had 62 clinical signs/symptoms. The most frequent are: Fatigue 97%,Hypermobility 95%, Arthralgia 95%, Finesse and skin transparency 94%, motordysproprioception 89%,Meno/metrorhaggia 87%, Bruisings 86% , Migraines 83%,Visual fatigue 83%, Plantar Contractions 82%, Dyspnea 82% Temperaturedysregulation 80%, Hyperacousia 79%, Increased skin stretching 79%, Sprains orpseudo-sprains 78%, Attention deficit 77%, Pseudo-Raynaud phenomenon 77%,Difficulty scarring 76%, Cutaneous hyperesthesia 76%, Genital pains 74%,Abdominal pains 74%, Gastroesophageal reflux 74%, Meteorism 74%, Hyperhidrosis73%, Decreased working memory capacity 73%; Hyperosmia 72%, Vertigo 71%.Each clinical problem was quantified by a 0-4 Likert scale before to be classifiedinto one of the following sections:- Axis 1 : Fragility of connective tissue - Skin, mucous membranes & teeth- Axis 2 : Fragility of Connective Tissue - Hemorrhagic Syndrome- Axis 3 : Proprioceptive disorders - Joints & motor skills- Axis 4 : Proprioceptive disorders - Dysautonomia- Axis 5 : Proprioceptive Disorders - Perception Disorders- Axis 6 : Alterations of cognitive functionsThe 62 items were also evaluated in the control groups included 826 healthysubjects and 206 patients with rheumatic conditions unrelated to EDSResults1-Comparison between the different axis.Statistical analysis showed that distributions of severity indices on 1, 3, 4 and 5 aresimilar and correlated two by two.The comparison between these groups disclosed a very significant dissociation withthe two other groups. Further, the 1, 3, 4 and 5 groups were very homogeneous.

This homogeneity is a strong argument in favor of the uniqueness of Ehlers-Danlosdisease and goes against its fragmentation into different types as suggested.2-Comparison between EDS patients and control groups (Heathly andGMS/General Medicine & Specialities)There is a very significant dissociation between the positioning of healthy controlsand MGS groups, on the one hand, and the SED patient group, on the other hand.We also note the very strong homogeneity of the EDS group. Indeed, by gatheringthe data in three categories, according to their severity (IEDS) of 0 to 8, one observesthe following distribution (in percentage for each group): IEDS 2: 7.3% of the EDSgroup, 97.1% of the MGS group and 99.6% of the control group, IEDS 2: 92.7% ofthe EDS group, 2.9% of the MGS group and 0.4% of the control group.The data allowed the design of a mathematical model that gives the EDS diagnosiswith a sensitivity of 99.6% and a specificity of 97,1% when the patient exhibits fiveout the following nine items: diffuse pains, fatigue, thin skin, proprioceptivemotor disorder, joint instability, hypermobility, gastroesophageal reflux, easybruising, and hyperacusis.

Specificity and sensitivity of the EDS quick diagnostic tool.Contribution of histology (electronic microscopy).Pr. Hermanns-Lê TrinhTwo hundred subjects with at least five out of the nine signs all had commonabnormalities of their dermal collagen network including variability in the diameter ofcollagen fibrils, flower-like collagen fibrils, and dense interstitial granulofilamentousdeposits.

*Hereditary transmission of EDSIf a father or a mother suffering from EDS, all children were also suffering from EDS.Recently, we verify that with 45 families examined in ELLAsanté Center in Paris.Conclusions

Our clinical algorithm enables EDS diagnosis early and with certainty. It hasseveral potential advantages. For instance, it might help confirm the hereditarycharacter of EDS, it might too obtain specific treatments and social supports, anddeny false accusations of parental abuse (in forensic medicine).Bibliography1-Hamonet Cl., P. Ravaud, S. Villeneuve, A. Gompel,. Fredy & all.Ehlers-Danlos. Etude statistique des symptômes et signes de 644 cas ayant un score deBeighton égal ou supérieur à 4/9. Premier Symposium international sur le syndromed’Ehlers-Danlos, 8-11 Septembre 2012, Ghent, Belgium.2-Trinh Hermanns-Lê, Daniel Manicourt, Biopsie cutanée dans le syndrome d'EhlersDanlos, troisième colloque international les traitements du syndrome d'Ehlers-Danlos;Université Paris-Descartes, Paris Mars 2017.3-Hamonet C, Brissot R., Anne Gompel A., Baeza-Velasco C., Guinchat V., Brock I.,Ducret L., Pommeret S. Metlaine A., Ehlers-Danlos Syndrome (EDS) - Contribution toClinical Diagnosis - A Prospective Study of 853 Patients.4-Hamonet Cl., preface by the Professeur Rodney Grahame (Londres): Ehlers-Danlos.La maladie oubliée par la médecine, Ehlers-Danlos. The disease forgotten by medicine,L'Harmattan, Paris, 2018.55-Four International colloquia in Paris, Ehlers-Danlos and its treatments: UniversityParis east Créteil: marsh 2015, marsh 2016, University Paris-Descartes marsh 2017,University Paris-Sorbonne (Salpetrière hospital about Cognitive and psychopathologicaspects) marsh 2018.Thanks to Doctor:Lucette Ducret for her efficient help

Ehlers-Danlos. Etude statistique des symptômes et signes de 644 cas ayant un score de Beighton égal ou supérieur à 4/9. Premier Symposium international sur le syndrome d’Ehlers-Danlos, 8-11 Septembre 2012, Ghent, Belgium. 2-Trinh Hermanns-Lê, Daniel Manicourt, Biopsie cutanée dans le syndrome d'Ehlers-

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