BACKGROUND: Glomuvenous malformations (GVMs) are now considered a separate entity from venous malformations. The rarest type of GVM is the generalized congenital plaque-type GVM. OBSERVATIONS: We present 10 new cases of congenital plaque-type GVM and describe their clinical progression and treatment. Mutations in the glomulin gene were found in those patients who participated in the genetic study. CONCLUSIONS: Congenital plaque-type GVMs are unique in their congenital nature, extensive distribution, difficult to diagnose and treat, and progressive involvement after birth. Most cases are familial, yet affected relatives usually have only minor lesions. The lesions of congenital plaque-type GVM are severe, visible at birth, and usually mistaken for extensive venous malformations. Vascular malformations are divided by hemodynamic type into slow-flow and fast-flow lesions. Slow-flow lesions are subcategorized as capillary, lymphatic, and venous.(1) Capillary malformations are flat, sharply demarcated, red-pink vascular stains of the skin commonly referred to as port-wine stains. These persist throughout life and are characterized histologically by dilated capillaries within the dermis. They slowly increase in size with age. Lymphatic malformations are spongelike collections of abnormal channels and spaces that contain clear lymphatic fluid, causing an excess of fluid to accumulate and dilate the lymphatic channels. This results in swelling of the affected area and, if extensive, can cause enlargement of soft tissues and bones.
BACKGROUND:Glomuvenous malformations (GVMs) are now considered a separate entity from venous malformations. The rarest type of GVM is the generalized congenital plaque-type GVM. OBSERVATIONS: We present 10 new cases of congenital plaque-type GVM and describe their clinical progression and treatment. Mutations in the glomulin gene were found in those patients who participated in the genetic study. CONCLUSIONS: Congenital plaque-type GVMs are unique in their congenital nature, extensive distribution, difficult to diagnose and treat, and progressive involvement after birth. Most cases are familial, yet affected relatives usually have only minor lesions. The lesions of congenital plaque-type GVM are severe, visible at birth, and usually mistaken for extensive venous malformations. Vascular malformations are divided by hemodynamic type into slow-flow and fast-flow lesions. Slow-flow lesions are subcategorized as capillary, lymphatic, and venous.(1) Capillary malformations are flat, sharply demarcated, red-pink vascular stains of the skin commonly referred to as port-wine stains. These persist throughout life and are characterized histologically by dilated capillaries within the dermis. They slowly increase in size with age. Lymphatic malformations are spongelike collections of abnormal channels and spaces that contain clear lymphatic fluid, causing an excess of fluid to accumulate and dilate the lymphatic channels. This results in swelling of the affected area and, if extensive, can cause enlargement of soft tissues and bones.
Authors: P Brouillard; L M Boon; N Revencu; J Berg; A Dompmartin; J Dubois; M Garzon; S Holden; L Kangesu; C Labrèze; S A Lynch; C McKeown; R Meskauskas; I Quere; S Syed; P Vabres; M Wassef; J B Mulliken; M Vikkula Journal: Mol Syndromol Date: 2013-03-26
Authors: Kyle E Robinson; Ali D Tahbouh Amawi; Sudhakar K Venkatesh; Jorge Torres-Mora; Ellen West; Amanika Kumar Journal: Gynecol Oncol Rep Date: 2022-06-24
Authors: Raja Shaikh; Ahmad I Alomari; John B Mulliken; Steven J Fishman; Harry P W Kozakewich; Gulraiz Chaudry Journal: Skeletal Radiol Date: 2014-02-28 Impact factor: 2.199
Authors: Mustapha Amyere; Virginie Aerts; Pascal Brouillard; Brendan A S McIntyre; François P Duhoux; Michel Wassef; Odile Enjolras; John B Mulliken; Olivier Devuyst; Hélène Antoine-Poirel; Laurence M Boon; Miikka Vikkula Journal: Am J Hum Genet Date: 2013-01-31 Impact factor: 11.025