Ehlers Danlos Syndrome

Clinical meaning

Ehlers-Danlos syndromes (EDS) are a heterogeneous group of heritable connective tissue disorders caused by genetic defects in collagen synthesis, structure, or processing. Collagen is the most abundant protein in the human body, providing structural integrity to skin, blood vessels, joints, organs, and virtually all connective tissues. Normal collagen biosynthesis involves transcription of procollagen alpha chains, hydroxylation of proline and lysine residues (requiring vitamin C as cofactor), triple helix formation, secretion, extracellular cleavage of propeptides, and cross-linking into mature collagen fibrils. EDS subtypes result from mutations affecting different steps in this pathway or different collagen types. The most common subtype, hypermobile EDS (hEDS), has no identified causative gene and is diagnosed clinically; the genetic basis likely involves multiple genes affecting extracellular matrix organization. Classical EDS (cEDS) results from mutations in COL5A1 or COL5A2 (type V collagen), causing defective collagen fibril assembly with characteristic skin hyperextensibility, atrophic scarring, and joint hypermobility. Vascular EDS (vEDS) -- the most dangerous subtype -- is caused by mutations in COL3A1 (type III collagen), which is the predominant collagen of blood vessel walls, hollow organs, and the uterus; deficient type III collagen leads to fragile arterial walls prone to spontaneous dissection and rupture, and hollow organ perforation. The Beighton score (0-9 points) quantifies generalized joint hypermobility by testing bilateral passive dorsiflexion of the 5th metacarpophalangeal joint beyond 90°, bilateral passive apposition of the thumb to the forearm, bilateral hyperextension of the elbow beyond 10°, bilateral hyperextension of the knee beyond 10°, and ability to place palms flat on the floor with knees locked. A score of ≥5/9 (≥4/9 for adults >50 years) indicates generalized joint hypermobility. The 2017 International Classification recognizes 13 EDS subtypes, each with specific clinical criteria and genetic testing recommendations.

Diagnosis & workup

Diagnostics & workup: - Beighton hypermobility score: standardized 9-point clinical assessment; ≥5/9 for adults ≤50 years, ≥4/9 for adults >50 years indicates generalized joint hypermobility; useful screening but NOT diagnostic of EDS alone -- must be combined with additional clinical criteria - 2017 International EDS Diagnostic Criteria for hEDS (all 3 criteria required): (1) Beighton score meeting threshold, (2) Two or more of: systemic connective tissue features (skin hyperextensibility, atrophic scarring, dental crowding, piezogenic papules, recurrent dislocations, chronic pain, positive family history), (3) Exclusion of other heritable connective tissue disorders - Genetic testing: indicated for suspected vEDS (COL3A1), cEDS (COL5A1/COL5A2), and other rare subtypes; NO genetic test exists for hEDS (clinical diagnosis only); next-generation sequencing panels covering connective tissue disorder genes - Echocardiography: screen for mitral valve prolapse (present in 6-25% of hEDS patients), aortic root dilation; annual echocardiography recommended for vEDS (monitor for aortic dissection and aneurysm) - Skin biopsy with electron microscopy: may show abnormal collagen fibril morphology (flower-like or cauliflower appearance in cEDS); not routinely diagnostic but useful in ambiguous cases - Vascular imaging (CT angiography or MR angiography): baseline vascular assessment for vEDS; identify aneurysms, dissections, or pseudoaneurysms; avoid invasive catheter-based angiography in vEDS (risk of arterial rupture from catheter) - Bone densitometry (DEXA): EDS patients have increased prevalence of osteopenia and osteoporosis due to defective collagen in bone matrix; early screening recommended

Risk factors: - Autosomal dominant inheritance for most subtypes (50% chance of transmission to offspring; cEDS, hEDS, and vEDS are all autosomal dominant; variable penetrance and expressivity within families) - Family history of hypermobility, easy bruising, chronic pain, or unexplained organ rupture (many families have undiagnosed EDS across generations) - Female sex: hEDS disproportionately affects females (8:1 ratio), possibly due to hormonal effects on connective tissue laxity; symptoms often worsen during puberty, menstruation, and pregnancy - Known COL3A1 mutation (vEDS): median survival 51 years; 25% of patients experience their first vascular or organ complication by age 20 - Associated conditions in hEDS: mast cell activation syndrome (MCAS), postural orthostatic tachycardia syndrome (POTS), and Chiari malformation type I form a recognized clinical triad - Pregnancy in vEDS: maternal mortality 5-12% per pregnancy from uterine or arterial rupture; pregnancy is considered high-risk and requires multidisciplinary management - Joint trauma from contact sports, repetitive strain, or physical therapy that exceeds joint stability capacity

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