histopathologic findings of microvascular occlusion syndromes

1
P7017 Histopathologic findings of microvascular occlusion syndromes Alicia Gonz alez-Quesada, MD, Hospital Universitario de Gran Canaria Dr. Negr ın, Las Palmas de Gran Canaria, Spain; Carolina Medina-Gil, MD, Hospital Universitario de Gran Canaria Dr. Negr ın, Las Palmas de Gran Canaria, Spain; Elena Castro-Gonz alez, MD, Hospital Universitario de Gran Canaria Dr. Negr ın, Las Palmas de Gran Canaria, Spain; Gregorio Carretero-Hern andez, MD, Hospital Universitario de Gran Canaria Dr. Negr ın, Las Palmas de Gran Canaria, Spain; Jaime Vilar-Alejo, MD, Hospital Universitario de Gran Canaria Dr. Negr ın, Las Palmas de Gran Canaria, Spain; Javier G omez-Duaso, MD, Hospital Universitario de Gran Canaria Dr. Negr ın, Las Palmas de Gran Canaria, Spain; Pedro Valer on- Almaz an, MD, Hospital Universitario de Gran Canaria Dr. Negr ın, Las Palmas de Gran Canaria, Spain A wide spectrum of systemic disorders may cause occlusion of the blood vessels. Cutaneous infarction only occurs when numerous vessels in the lower dermis and subcutis are occluded. The differential diagnosis for microvascular syndromes involving the skin is extensive, and the evaluation may be difficult as they can share similar signs and symptoms. Clinical manifestations may include non inflamatory purpura without erythtema, necrotic eschars, branching, cutaneous infarction, retiform purpura or livedo reticularis. Based on pathophysiology, microvascular occlusion syndromes may classified in platelet plugging (eg, heparin necrosis or myeloproliferative disorders), emboli or crystal deposition (eg, cholesterol emboli), vascular coagulopathies, abnormal proteins deposition (eg, cryoproteinemia) or septic embolisms. We present a case series of different microvascular syndromes, including cryoglobulinemia, cholesterol embolism, septic embolism and calciphy- laxis. Although these patients showed different clinical presentations among the typical symptoms of microvascular syndromes, the cutaneous biopsy could help in the identification of the underlying process of each case. We would like to hightlight the importance of the histopathological examination in microvascular occlusion syndromes in order to achive an accurate diagnosis. Commercial support: None identified. P6764 Human piebaldism Taciana Rocha de Hollanda, MD, Universidade Federal do Rio de Janeiro, Rio de Janeiro, Brazil; Juliany Estefan, MD, Universidade Federal do Rio de Janeiro, Rio de Janeiro, Brazil; Manuela Boleira, MD, Policlinica Geral do Rio de Janeiro, Rio de Janeiro, Brazil; Marcia Ribeiro, PhD, MD, Universidade Federal do Rio de Janeiro, Rio de Janeiro, Brazil Human piebaldism is a rare autosomal dominant disorder caused by defective melanoblast proliferation and migration during embryogenesis. Affected individuals present at birth with areas of leukoderma which are achromic and melanocytes are not present in such areas. We present a case of a 4-month-old girl who presented at birth achromic patches on inferior limbs and periumbilical region with small islands of hyperpigmentation and a white forelock. She had no other abnormalities on physical examination. There was no familiar consanguinity. A paternal lineage of affected individuals was observed: great grandfather, grandfather, 3 aunts, 1 uncle and a 3-year old sister showed the same achromic patches. Her father, although affected, did not present achromic areas, but hypochromic one. The familial occurrence, in which more than one generation is affected; with no sex preference, is compatible with an autosomal dominant inheritance with incomplete penetrance and variable expressivity. Molecular studies of this family will help understanding the mechanisms on this rare disorder. Commercial support: None identified. P6360 Identification of a novel ECM1 mutation in 2 siblings with lipoid proteinosis Etienne Saint-Cyr Proulx, MD, MS, Center Hospitalier de l’Universit e de Montr eal, Quebec, Canada; Fatemeh Jafarian, MD, McGill University Health Center, Montr eal, Quebec, Canada Lipoid proteinosis is a rare autosomal recessive genodermatosis characterized by the deposition of hyaline material in the skin, mucosa, internal organs, and central nervous system. It is caused by loss-of-function mutations in the extracellular matrix protein 1 gene (ECM1). No effective therapy has been described for this condition yet. A 16-year-old boy was referred to our center with a history of severe long-standing acne-like scarring. The lesions had started in late infancy and had progressed during childhood. The patient’s parents were first cousins and a younger brother suffered from a similar problem. The physical examination of both siblings revealed pock-like scars on the face, trunk, and upper extremities as well as beaded papules lining the eyelids. Generalized thickening of the skin was seen in the elder sibling only. Both patients’ voices were remarkably hoarse. Investigations including complete blood count, serum biochemistry, EEG, brain MRI, and laryngoscopic examination were all within normal limits. A skin biopsy revealed hyaline deposition in the papillary dermis and surrounding the blood vessels, adnexal epithelia and dermoepidermal junction. Electron microscopy showed thickened vessel walls with embedded pericytes and irregular concentric duplication of the basement membranes. The diagnosis of lipoid proteinosis was confirmed by genetic analysis which revealed a novel homozygous non-sense mutation in exon 9 of the ECM1 gene. Both patients were started on acitretin at 0.5 mg/kg/day. The treatment was well tolerated, but no objective or subjective improvement of the skin lesions or hoarseness were noted after 6 months. The treatment was discontinued. Although previous studies have reported improvement of skin lesions and hoarseness with acitretin, our results were negative. As is the case for all rare diseases, large randomized studies are not feasible and the search for an effective therapeutic option relies on trial and error. Further research into the pathophys- iology of lipoid proteinosis will hopefully provide insight to guide future therapeutic trials. Commercial support: None identified. P6271 IQoL: A new ichthyosis-specific measure of quality of life Juliette Mazereeuw-Hautier, MD, Reference Center for rare skin diseases, Toulouse, France; A. Maza, MD, Reference Center for Rare Skin Diseases, Toulouse, France; Charles-Remy Taieb, MD, MBA, CREES PFSA, Boulogne Billancourt, France; E. Bourrat, MD, H^ opital Saint-Louis, Paris, France; I. Galera, MD, Reference Center for Rare Skin Diseases, Toulouse, France; Isabelle Dreyfus, PharmD, Reference Center for Rare Skin Diseases, Toulouse, France; S ebastien Barbarot, MD, Department of Dermatology, NANTES, France Background: Congenital ichtyoses are associated with impaired quality of Life (QoL). In order to explore the facets of this disease and monitor changes in QoL, a specific tool was needed. The aim of this study was therefore to create and validate a specific QoL questionnaire. Methods: Focus groups worked on a first list of items. After streamlining these items, a prequestionnaire (Q) was drawn up and subjected to a cognitive debriefing. During the validation phase, this Q (together with the DLQI, SF-12, and severity) was sent to patients aged 15 and over, suffering from ichtyosis of varying forms and severities. A shortened version of the Q was designed by removing repetitive items and those identified by the analysis as not having an impact on the score. The validity of the tool was confirmed: both for its structure and one-dimensional nature (Cronbach a), convergent (Spearman correlation) and discriminating validity (Tukey test); a fixed at 5%. The English version of this questionnaire has been validated. Results The initial Q comprised 60 items. During the validation phase, 59 subjects were tested. The shortened version included 32 Items (IQoL-32) and 7 dimensions (Cronbach 0.94). The higher the score, the more impacted is the QoL. IQoL-32 is positively correlated to the DLQI (P \.0001) and the SF-12 (P \.0001). IQoL-32 is highly correlated to the clinical severity: overall analysis (Spearman ranking: 0.72; P \ .0001, same for the 7 dimensions (highest correlations: discomfort, pain, interpersonal relations). IQoL-32 demonstrated a higher correla- tion with VAS compared with the DLQI and the SF-12. It also showed a good discriminating power (P \.0001) according to overall severity levels (scores were higher especially when severity levels were too). Discussion: This study helped design the very first specific questionnaire on congenital ichtyosis. Based on a validated method, the IQoL-32 is simple to use in clinical practice and research. It is more sensitive than DLQI or SF-12 when assessing the QoL of ichtyosis sufferers. Study population included patients with ichtyosis of varying forms and severities. These patients were either receiving hospital outpa- tient care or were members of the patients’ association. This Q can therefore be used in all ichtyosis forms. Conclusion: This specific QoL scale will be a very useful tool for improving the management of patients with congenital ichtyosis. Commercial support: None identified. AB98 JAM ACAD DERMATOL APRIL 2013

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Page 1: Histopathologic findings of microvascular occlusion syndromes

P7017Histopathologic findings of microvascular occlusion syndromes

Alicia Gonz�alez-Quesada, MD, Hospital Universitario de Gran Canaria Dr. Negr�ın,Las Palmas de Gran Canaria, Spain; Carolina Medina-Gil, MD, HospitalUniversitario de Gran Canaria Dr. Negr�ın, Las Palmas de Gran Canaria, Spain;Elena Castro-Gonz�alez, MD, Hospital Universitario de Gran Canaria Dr. Negr�ın,Las Palmas de Gran Canaria, Spain; Gregorio Carretero-Hern�andez, MD, HospitalUniversitario de Gran Canaria Dr. Negr�ın, Las Palmas de Gran Canaria, Spain;Jaime Vilar-Alejo, MD, Hospital Universitario de Gran Canaria Dr. Negr�ın, LasPalmas de Gran Canaria, Spain; Javier G�omez-Duaso, MD, Hospital Universitariode Gran Canaria Dr. Negr�ın, Las Palmas de Gran Canaria, Spain; Pedro Valer�on-Almaz�an, MD, Hospital Universitario de Gran Canaria Dr. Negr�ın, Las Palmas deGran Canaria, Spain

A wide spectrum of systemic disorders may cause occlusion of the blood vessels.Cutaneous infarction only occurs when numerous vessels in the lower dermis andsubcutis are occluded. The differential diagnosis for microvascular syndromesinvolving the skin is extensive, and the evaluation may be difficult as they can sharesimilar signs and symptoms. Clinical manifestations may include non inflamatorypurpura without erythtema, necrotic eschars, branching, cutaneous infarction,retiform purpura or livedo reticularis. Based on pathophysiology, microvascularocclusion syndromes may classified in platelet plugging (eg, heparin necrosis ormyeloproliferative disorders), emboli or crystal deposition (eg, cholesterol emboli),vascular coagulopathies, abnormal proteins deposition (eg, cryoproteinemia) orseptic embolisms. We present a case series of different microvascular syndromes,including cryoglobulinemia, cholesterol embolism, septic embolism and calciphy-laxis. Although these patients showed different clinical presentations among thetypical symptoms of microvascular syndromes, the cutaneous biopsy could help inthe identification of the underlying process of each case. Wewould like to hightlightthe importance of the histopathological examination in microvascular occlusionsyndromes in order to achive an accurate diagnosis.

AB98

cial support: None identified.

Commer

P6764Human piebaldism

Taciana Rocha de Hollanda, MD, Universidade Federal do Rio de Janeiro, Rio deJaneiro, Brazil; Juliany Estefan, MD, Universidade Federal do Rio de Janeiro, Riode Janeiro, Brazil; Manuela Boleira, MD, Policlinica Geral do Rio de Janeiro, Riode Janeiro, Brazil; Marcia Ribeiro, PhD, MD, Universidade Federal do Rio deJaneiro, Rio de Janeiro, Brazil

Human piebaldism is a rare autosomal dominant disorder caused by defectivemelanoblast proliferation and migration during embryogenesis. Affected individualspresent at birth with areas of leukoderma which are achromic and melanocytes arenot present in such areas. We present a case of a 4-month-old girl who presented atbirth achromic patches on inferior limbs and periumbilical region with small islandsof hyperpigmentation and a white forelock. She had no other abnormalities onphysical examination. There was no familiar consanguinity. A paternal lineage ofaffected individuals was observed: great grandfather, grandfather, 3 aunts, 1 uncleand a 3-year old sister showed the same achromic patches. Her father, althoughaffected, did not present achromic areas, but hypochromic one. The familialoccurrence, in which more than one generation is affected; with no sex preference,is compatible with an autosomal dominant inheritance with incomplete penetranceand variable expressivity. Molecular studies of this family will help understandingthe mechanisms on this rare disorder.

cial support: None identified.

Commer

J AM ACAD DERMATOL

P6360Identification of a novel ECM1 mutation in 2 siblings with lipoidproteinosis

Etienne Saint-Cyr Proulx, MD, MS, Center Hospitalier de l’Universit�e de Montr�eal,Quebec, Canada; Fatemeh Jafarian, MD, McGill University Health Center,Montr�eal, Quebec, Canada

Lipoid proteinosis is a rare autosomal recessive genodermatosis characterized bythe deposition of hyaline material in the skin, mucosa, internal organs, andcentral nervous system. It is caused by loss-of-function mutations in theextracellular matrix protein 1 gene (ECM1). No effective therapy has beendescribed for this condition yet. A 16-year-old boy was referred to our center witha history of severe long-standing acne-like scarring. The lesions had started in lateinfancy and had progressed during childhood. The patient’s parents were firstcousins and a younger brother suffered from a similar problem. The physicalexamination of both siblings revealed pock-like scars on the face, trunk, andupper extremities as well as beaded papules lining the eyelids. Generalizedthickening of the skin was seen in the elder sibling only. Both patients’ voiceswere remarkably hoarse. Investigations including complete blood count, serumbiochemistry, EEG, brain MRI, and laryngoscopic examination were all withinnormal limits. A skin biopsy revealed hyaline deposition in the papillary dermisand surrounding the blood vessels, adnexal epithelia and dermoepidermaljunction. Electron microscopy showed thickened vessel walls with embeddedpericytes and irregular concentric duplication of the basement membranes. Thediagnosis of lipoid proteinosis was confirmed by genetic analysis which revealeda novel homozygous non-sense mutation in exon 9 of the ECM1 gene. Bothpatients were started on acitretin at 0.5 mg/kg/day. The treatment was welltolerated, but no objective or subjective improvement of the skin lesions orhoarseness were noted after 6 months. The treatment was discontinued.Although previous studies have reported improvement of skin lesions andhoarseness with acitretin, our results were negative. As is the case for all rarediseases, large randomized studies are not feasible and the search for an effectivetherapeutic option relies on trial and error. Further research into the pathophys-iology of lipoid proteinosis will hopefully provide insight to guide futuretherapeutic trials.

cial support: None identified.

Commer

P6271IQoL: A new ichthyosis-specific measure of quality of life

Juliette Mazereeuw-Hautier, MD, Reference Center for rare skin diseases,Toulouse, France; A. Maza, MD, Reference Center for Rare Skin Diseases,Toulouse, France; Charles-Remy Taieb, MD, MBA, CREES PFSA, BoulogneBillancourt, France; E. Bourrat, MD, Hopital Saint-Louis, Paris, France; I. Galera,MD, Reference Center for Rare Skin Diseases, Toulouse, France; Isabelle Dreyfus,PharmD, Reference Center for Rare Skin Diseases, Toulouse, France; S�ebastienBarbarot, MD, Department of Dermatology, NANTES, France

Background: Congenital ichtyoses are associated with impaired quality of Life (QoL).In order to explore the facets of this disease and monitor changes in QoL, a specifictool was needed. The aim of this studywas therefore to create and validate a specificQoL questionnaire.

Methods: Focus groupsworked on a first list of items. After streamlining these items,a prequestionnaire (Q) was drawn up and subjected to a cognitive debriefing.During the validation phase, this Q (together with the DLQI, SF-12, and severity) wassent to patients aged 15 and over, suffering from ichtyosis of varying forms andseverities. A shortened version of the Q was designed by removing repetitive itemsand those identified by the analysis as not having an impact on the score. The validityof the tool was confirmed: both for its structure and one-dimensional nature(Cronbach a), convergent (Spearman correlation) and discriminating validity(Tukey test); a fixed at 5%. The English version of this questionnaire has beenvalidated. Results The initial Q comprised 60 items. During the validation phase, 59subjects were tested. The shortened version included 32 Items (IQoL-32) and 7dimensions (Cronbach 0.94). The higher the score, the more impacted is the QoL.IQoL-32 is positively correlated to the DLQI (P\.0001) and the SF-12 (P\.0001).IQoL-32 is highly correlated to the clinical severity: overall analysis (Spearmanranking: 0.72; P \ .0001, same for the 7 dimensions (highest correlations:discomfort, pain, interpersonal relations). IQoL-32 demonstrated a higher correla-tion with VAS compared with the DLQI and the SF-12. It also showed a gooddiscriminating power (P\.0001) according to overall severity levels (scores werehigher especially when severity levels were too).

Discussion: This study helped design the very first specific questionnaire oncongenital ichtyosis. Based on a validated method, the IQoL-32 is simple to use inclinical practice and research. It is more sensitive than DLQI or SF-12when assessingthe QoL of ichtyosis sufferers. Study population included patients with ichtyosis ofvarying forms and severities. These patients were either receiving hospital outpa-tient care orweremembers of the patients’ association. This Q can therefore be usedin all ichtyosis forms.

Conclusion: This specific QoL scale will be a very useful tool for improving themanagement of patients with congenital ichtyosis.

cial support: None identified.

Commer

APRIL 2013