Hypermobile Ehlers Danlos Syndrome

Diagnostic Criteria

hEDS is a clinical spectrum from asymptomatic joint hypermobility, to “non syndromic” hypermobility, to hEDS. The latest diagnostic criteria for hEDS were published in 2017 ^[1]

hEDS Diagnostic Criteria Checklist

Summary

Criterion 1: Generalised Joint Hypermobility

Criterion 2: At least 2 features must be present

Criterion 3: All three prerequisites must be met

Beighton Scoring System (See Picture)

Motion	Negative	Unilateral	Bilateral
Passive dorsiflexion of the 5th finger >90 degrees	0	1	2
Passive flexion of the thumbs to the forearms	0	1	2
Hyperextension of the elbows >10 degrees	0	1	2
Hyperextension of the knees >10 degrees	0	1	2
Forward flexion of the trunk with knees fully extended and palms resting on the floor	0	1

Must meet Beighton Score for age

Age	Beighton Score
Prepubescent or adolescent	≥6
Pubescent up until age 50	≥5
Over age 50	≥4
Patients with Acquired joint limitations	BS 1 point under age requirements AND a positive 5PQ

Five Point Questionnaire for identifying hypermobility (5PQ)
Criteria: Two or more “yes” answers suggest joint hypermobility.
Can you now (or could you ever) place your hands flat on the floor without bending your knees? Can you now (or could you ever) bend your thumb to touch your forearm? As a child, did you amuse your friends by contorting your body into strange shapes, or could you do the splits? As a child or teenager, did your shoulder or kneecap dislocate on more than one occasion? Do you consider yourself double jointed?

Feature A: Systemic manifestations of CTD (need ≥5)'

1. Unusually soft/velvety skin
2. Mild skin hyperextensibility
3. Unexplained striaedistensae/rubrae
4. Bilateral piezogenic papules of heel
5. Recurrent/multiple abdominal hernia
6. Atrophic scaring in ≥2 sites
7. Pelvic floor, rectal, and/or uterine prolapse in children, men or nulliparous women
8. Dental crowding and high or narrow palate
9. Arachnodactyly
10. Arm span-to-height ≥1.05
11. Mitral valve prolapse
12. Aortic root dilatation with Z score > +2

Skin extensibility as measured by pinching and lifting the cutaneous and subcutaneous layers of the skin on the volar surface at the middle of the non-dominant forearm as described in Remvig et al, 2009. Skin extensibility of >1.5 cm is considered the upper end of normal. It is likely that the hyperextensibility of the skin in hEDS overlaps significantly with that of “normal” skin. Therefore, extensibility of more than 1.5 cm is “positive.” If extensibility >2.0 cm is present especially in combination with other cutaneous features, such as papyraceous scars, molluscoid pseudotumors and/or subcutaneous spheroids, consider other EDS types as possible alternative diagnoses (mainly cEDS and classical-like EDS)

Feature B: Family history (1 or more first-degree relatives must meet criteria)

Feature C: MSK Complications(need ≥1)

1. MSK pain in ≥2 limbs, recurring daily for ≥3 months
2. Chronic widespread pain for ≥3 months
3. Recurrent joint dislocations or frank joint instability, in the absence of trauma (a or b)
   • ≥3 atraumatic dislocations in same joint or ≥2 more atraumatic dislocations in two difference joints occurring at different times
   • Medical confirmation of joint instability at two or more sites not related to trauma

Skin hyperextensibility and Generalized Joint Hypermobility on physical exam^[2]

1. Absence of unusual skin fragility.
2. Exclusion of other heritable and acquired connective tissue disorders. In patients with an acquired onnective tissue disorder, additional diagnosis of hEDS requires meeting both Features A and B of Criterion 2. Feature C of Criterion 2 cannot be counted in this situation.
3. Exclusion of alternative diagnoses that may also include joint hypermobility by means of hypotonia and/or connective tissue laxity

Controversies

The first problem is that the Beighton scoring method for assessing generalised hypermobility is highly flawed and has garnered some controversy. Some authors argue for a greater emphasis on clinician judgement.^[3]

The hEDS subtype of EDS has varying levels of acceptance and awareness as a diagnostic entity by various relevant specialists in New Zealand. What some clinicians diagnose as hEDS, some clinicians may instead diagnose Fibromyalgia, another controversial condition that is not commonly diagnosed in Musculoskeletal Medicine, benign joint hypermobility syndrome plus fibromyalgia, or simply Central Sensitisation which again has controversies.

The evidence for applying any one or more of the above diagnoses is not robust. Some of the controversy stems from the lack of clearly objective tests. hEDS, fibromyalgia, Benign Joint Hypermobility Syndrome, and central sensitisation are all diagnosed using subjective "committee criteria" or "questionnaires." Committee diagnoses are when a group of experts come together to publish a list of symptoms and signs, and that if you fulfill those symptoms you have the disorder. There is always a but; committee diagnoses always stipulate that other conditions must be excluded first. Therefore it is not logically possible to choose between one committee diagnosis and the other (e.g. hEDS and fibromyalgia) when the patient fulfills the criteria for both conditions for the same symptoms. In the absence of widely accepted objective test and the removal of the "exclude other conditions" stipulation, who is to say that hEDS trumps fibromyalgia, or that fibryomyalgia trumps hEDS? Furthermore how does one accurately differentiate between primary chronic widespread pain versus pain with joint laxity?

The existence of a committee diagnosis for a condition does not in itself mean that the condition doesn't exist. Migraine, or the entire field of psychiatric diagnoses are good examples of mainstream committee diagnoses that have broad acceptance. Glioblastoma and myocardial infarction are good examples of a more objective diagnoses. The subjective nature of diagnosis can lead to poor inter-observer reliability and can fuel the flame of controversy.

There is some conflict between Benign Joint Hypermobility Syndrome (BJHS) and hypermobile Ehlers Danlos Syndrome. The former is diagnosed using the 1998 Brighton criteria and has come from the Rheumatology literature, which is probably why it is favoured by some Rheumatologists. Hypermobile Ehlers Danlos Syndrome is diagnosed using the 2017 diagnostic criteria and comes from the Genetics and Paediatrics literature. Some authors and clinicians believe that these two conditions are in fact the same thing.

Patients in whom this or related diagnoses are being considered are clearly suffering and have very real symptoms. Clinicians may of course make such diagnoses, and indeed they do so regularly. Making a committee diagnosis can be helpful in framing and providing a narrative through which to support management in a patient centered model of care. Medical discoveries are all made through trying new things, and as long as the patient is fully informed then the clinician and patient may wish to explore hEDS as a framework.

However at the extreme it can lead to polypharmacy, perpetuate the cycle of hope and despair, and the patient may experience resentment from some health care providers who do not "believe" in the disorder. One should always keep in mind the limitations of the diagnostic criteria and treatment evidence, the socio-psychological factors, the potential benefits and harms of making the diagnosis, and the context of the broader healthcare system.

Triad of hEDS, MCAS, and POTS

Some patients with hEDS may also be diagnosed with mast cell activation syndrome (MCAS) and postural orthostatic tachycardia syndrome (POTS). Kohn et al evaluated the literature behind each of these three conditions, and the relationship between them^[4]. They concluded that there is no proven relationship between hypermobile Ehlers Danlos Syndrome, Mast Cell Activation Syndrome, and POTS, and no proven pathophysiological mechanism linking them. The main limitation of their review was that most of the studies to date used the older criteria of hEDS which was much more inclusive and more vague, making analysis more difficult. They theorised that the reason that these conditions have been associated is because there is a large overlap of non-specific symptomatology, summarised in their Venn Diagram below. Please note that MCAS as a diagnostic entity is controversial and only minority support in New Zealand.^[5]

Differential Diagnosis

• Generalised Joint Hypermobility
• Hypermobility Spectrum Disorder or Hypermobile Ehlers Danlos Syndrome
• Ehlers Danlos Syndrome
• Marfan Syndrome
• Osteogenesis Imperfecta Type 1
• Geroderma Osteodysplasticum
• Loeys-Dietz
• Arterial Tortuosity Syndrome
• Lateral Meningocele Syndrome
• Bethlem Myopathy
• Ullrich congenital muscular dystrophy
• Acromesomelic Dysplasia
• Coffin-Lowry Syndrome
• Cohen Syndrome
• Cranioectodermal Dysplasia
• Deletion 2q37 Syndrome
• Down Syndrome
• Floating-Harbor Syndrome
• Hajdu-Cheney Syndrome
• Kabuki Syndrome
• Loeys-Dietz Syndrome
• Macrocephaly-Capillary Malformation
• Meier-Gorlin Syndrome
• Metatropic Dysplasia
• Microcephalic Primordial Dwarfing Syndrome
• Microdeletion 15q24 Syndrome
• Microdeletion 22q11.2 Syndrome
• Morquio Syndrome
• Multiple Endocrine Neoplasia Type 2B
• Peters'-Plus Syndorme
• Pitt-Hopkins Syndrome
• Pseudoachondroplasia
• SHORT Syndrome
• Stickler Syndrome
• 3-M Syndrome
• XXXY and XXXXY SDyndrome

Resources

hEDS Diagnostic Criteria Checklist - 158 KB (f)

One page checklist for hEDS

EDS Classifications 2017 - 896 KB (f)

Full diagnostic criteria of all EDS subtypes

The relationship between hEDS, POTS, and MCAS - 1.18 MB (f)

Interesting critique by Kohn et al (2019) on the assumption that these conditions are linked

• Dr Matthew Preston | Ehlers-Danlos Syndromes (matpre.nz)
• Ehlers-Danlos Syndrome (EDS) Algorithm and Resources for Primary Care - Mountain States GeneticsMountain States Genetics
• The Ehlers-Danlos syndromes (EDS) GP Toolkit

References

Papers of particular interest have been highlighted as: ◆ of special interest ◆◆ of outstanding interest

Literature Review