Musculoskeletal

Question 1

What is the definition and epidemiology of Amyloidosis?

Answer 1

Amyloidosis is a group of diseases in which abnormal protein, known as amyloid fibrils, build up in tissue. There are about 30 different type of amyloidosis, each due to a specific protein mis-folding. Deposits of amyloid may be localised in tissue or part of a systemic process. It is quite rare, with 60 new cases a year. Median age is 64 years at diagnosis, but patients can present at any age.

Question 2

What is the aetiology of Amyloidosis?

Answer 2

Primary amyloidosis is also known as immunoglobulin light chain amyloidosis. It is similar to multiple myeloma in the sense that it involves clonal plasma cells releasing light chains. However there is a distinction in the percentage of plasma cells in the bone marrow. Less than 0.5% of amyloid patients go on to develop multiple myeloma during the course of their disease.

Secondary amyloidosis can be divided into familial and non-familial:
Non-familial:
○ Inflammatory polyarthropathies account for 60% of cases. Conditions include rheumatoid arthritis, juvenile arthritis, psoriatic arthritis and ankylosing spondylitis.
○ Chronic infections such as bronchiectasis, subcutaneous injection of illicit drugs, decubitus ulcers, chronic UTIs and osteomyelitis.
○ Inflammatory bowel disease specifically Crohn’s disease can result in secondary amyloidosis.
○ Castleman’s disease is a lymphoproliferative disorder where the plasma cell variant can cause secondary amyloidosis.

Familial is caused by familial mediterranean fever, TNF receptor-associated periodic fever syndromes, Muckle-Wells syndrome, Hyper-IgD syndrome.

Question 3

What are the clinical features of Amyloidosis?

Answer 3

Presentation is broad and depends on the site of amyloid accumulation. The kidneys and heart are the most common organs involved.

Amyloid deposition in the kidneys can cause Nephrotic Syndrome. This presents as lower extremity oedema (due to Hypoalbuminaemia).

Amyloid deposition in the heart causes restrictive cardiomyopathy. This produces a raised JVP, as well as symptoms of heart failure such as fatigue, dyspnoea on exertion.

People with amyloidosis do not get CNS involvement but can develop sensory and autonomic neuropathies. These develop in a symmetrical pattern an progresses in a distal to proximal manner. Autonomic neuropathy can present as orthostatic hypotension, but manifest more gradually with nonspecific gastrointestinal symptoms like constipation, nausea, or early satiety.

Other key diagnostic features include periorbital purpura - present in 15% of patients - eyelid petechial are common, and macroglossia which may cause sleep apnoea.

Question 4

How can Amyloidosis be investigated?

Answer 4

Serum immunofixation and urine immunofixation can confirm the presence of monoclonal protein.

Immunoglobulin free light chain assay will show an abnormal kappa:lambda ratio. This test is relatively new but has a extremely high sensitivity.

Bone marrow biopsy is a good source of tissue, and shows clonal plasma cells.

Tissue biopsy can show the presence of amyloids. Seen as a positive green birefringence when stained with Congo red.

Question 5

What is the definition and epidemiology of Ankylosing Spondylitis?

Answer 5

Ankylosing Spondylitis is a chronic progressive inflammatory arthropathy commonly affecting the spine and sacroiliac joints. It is the most common of the seronegative spondyloarthropaties affecting 150 per 100 000. Affects men more than women 3:1, and peaks at ages 17-35.

Question 6

What is the aetiology of Ankylosing Spondylitis?

Answer 6

Caused by both genetic and environmental factors. Strongly genetic with heritability of 97%. HLA-B27 is the most common predisposing gene.

Question 7

What are the symptoms of Ankylosing Spondylitis?

Answer 7

As sacroiliac joint is usually affected first, patient present with dull back pain (radiating to the hips and buttocks) and stiffness for >6 months. The symptoms are worse at night and in the early morning and relieved by exercise and worsened by rest.

Soon after, there is also involvement of the spine (intervertebral disks, zygapophysial, costovertebral and costotransverse joints). This manifests as reduced motion in the lumbar spine and cervical spine movements can be globally reduced.

30% of patients complain of peripheral synovitis - typically asymmetrical oligoarthritis, most commonly affecting the hip and knee.

Patients also present with extra-articular features of AS. Most commonly (40%) present with iritis. Can also have apical lung fibrosis, aortic incopetence, AV node block, achilles tendinitis, and rarely amyloidosis.

Question 8

What are the examination features of Ankylosing Spondylitis?

Answer 8

• Note loss of lumbar lordosis and increased thoracic kyphosis and neck hyperextension (question mark posture).
• Reduced chest expansion due to progressive loss of spinal movements.

Question 9

How can Ankylosing Spondylitis be investigated?

Answer 9

Pelvic X-ray should be requested in all patients with inflammatory back pain. Sacroiliitis can be unilateral or bilateral, and graded from 1 to 4 on severity. The presence of sacroiliitis is a requirement for the diagnosis of AS (based on the modified New York classification criteria).

Bloods:
• FBC is normal
• ↑ESR and CRP in active disease
• RF and ANA negative
• HLA-B27 is positive in up to 95% of white patients with AS, but has little role in diagnosis, but may indicate a predisposition (as only 6.5% of patients with HLA-B27 will develop AS).

MRI spine may show early sacroiliitis and early inflammatory changes in the spine.

Thoracic, cervical and lumbar X-Ray (lateral) should be performed on all AS patients to give a baseline and monitor disease progression with. Late disease may show bamboo spine.

Question 10

What is the definition of Antiphospholipid syndrome?

Answer 10

Antiphospholipid syndrome is an autoimmune hypercoagulable state caused by antiphospholipid antibodies. APS provokes thrombosis in both arteries and veins as well as pregnancy-related complications such as miscarriage, stillbirth, preterm delivery and severe preeclampsia.

Question 11

What is the aetiology of Antiphospholipid syndrome?

Answer 11

APS can occur in patients without an underlying autoimmune disease (primary APS) . Secondary APS occurs with another autoimmune disease, most notably Systemic Lupus Erythromatosus but also Sjogren’s syndrome, rheumatoid arthritis, systemic sclerosis, etc. The actual incidence of APS is unknown, and the disorder is probably underdiagnosed.

Question 12

What are the clinical features of Antiphospholipid Syndrome?

Answer 12

Patients have a history of vascular thrombosis such as stroke, coronary artery thrombus, peripheral arterial disease, and renal thrombotic microangiopathy.

Female patients have a history of pregnancy loss, defined as three or more consecutive pregnancy losses <10 weeks’ gestation and/or unexplained foetal death >10 weeks’ gestation.

There may also be a history of pregnancy-associated morbidity such as premature delivery due to pre-eclampsia, placental abruption, growth restriction.

Patients also commonly present with features of thrombocytopaenia such as petechial rash or mucosal bleeding.

Question 13

How is Antiphospholipid syndrome investigated?

Answer 13

The antiphospholipid antibodies must be detected and elevated on 2 occasions, 12 weeks apart:
• Lupud anticoagulant
• Anticardiolipin antibodies
• Anti-beta2-glycoprotein I antibodies

ANA, dsDNA antibdoes are positive in SLE

FBC may show thrombocytopaenia.

Question 14

What is the definition and epidemiology of Behçet’s disease?

Answer 14

Behçet’s disease is a systemic vasculitis most commonly seen in Turkey, Israel, the Mediterranean basin, and eastern Asia. It can cause skin and mucsoal lesions, uveitis, major arterial and venous disease, and GI and neurological manifestations.

Question 15

What are the clinical features of Behçet’s disease?

Answer 15

As the vasculitis affects any organ, there are a wide variety of symptoms.

This commonly includes recurrent oral ulcers (related to apthous ulcers but are larger, more painful and take weeks to heal) as well as painful genital ulcers in the anus, vulva or scrotum.

Patients also complain of uveitis which may be painful presenting as a redness of conjunctiva and a decrease in vision. Posterior uveitis can present as a painless decrease in vision with visual field floaters.

Folliculitis and Erythema Nodosum are also common in the lower extremities.

There may also be bowel, lung, musculoskeletal (athralgia) and neurological involvement.

Question 16

How is Behçet’s disease investigated?

Answer 16

Importantly, the patient is RF, ANA and ANCA negative.

A skin pathergy test is performed where a subcutaneous skin prick is performed on a patient. Up to 60% of patients form a pustule within 48 hours.

Question 17

What is the definition and epidemiology of Carpal Tunnel Syndrome?

Answer 17

CTS is a collection of symptoms and signs caused by the compression of the medial nerve in the carpal tunnel. Quite common affecting 3.7% of the population.

Question 18

What are the risk factors for Carpal Tunnel Syndrome?

Answer 18

Risk factors include:
• Age over 30
• High BMI
• Female sex
• Alterations in carpal tunnel space
• Fractured wrist/carpal bones
• Square wrist
• Rheumatoid arthritis
• Diabetes
• Dialysis
• Pregnancy

Question 19

What are the clinical features of Carpal Tunnel Syndrome?

Answer 19

Patients present with a gradual onset numbness of hand(s). The dominant hand is usually the first and worst affected. Although the median nerve affects the palmar aspect of the first 4 fingers, patients usually complain of the whole hand going numb. Patients typically also complain of aching and pain in the arm.

Patients also commonly have weakness of the hand (particularly for rotational movements such as opening a jar). They may report this as clumsiness.

Symptoms are intermittent and worse at night-time.

Question 20

How can Carpal Tunnel Syndrome be investigated?

Answer 20

An EMG is the diagnostic test of choice. Shows a focal slowing of conduction velocity in the median sensory nerves across the carpal tunnel.

Ultrasound or MRI of the wrist may identify a space-occupying lesion.

Question 21

What is the definition and epidemiology of Fibromyalgia?

Answer 21

Fibromyalgia is a syndrome of chronic pain and the presence of hyperalgeic points at specific anatomical sites, as well as a range of other physical and psychological symptoms with no identifiable organic cause. It is 10x more common in women, and affects individuals aged 20-50. It is quite common affecting 2-4% of the general population, but is often underdiagnosed.

Question 22

What is the aetiology of Fibromyalgia?

Answer 22

The cause is poorly understood, but abnormal central and peripheral pain processing is thought to be responsible for reduced pain threshold, hyperalgesia and allodynia (pain produced by non-noxious stimulus). Associated with physical trauma (e.g. whiplash), psychological trauma such as stress, anxiety and depression, as well as post-viral infection.

Question 23

What are the clinical features of Fibromyalgia?

Answer 23

Patients present with:
• Fatigue unrelieved by rest
• Insomnia, Irritability, Irritable bowel and irritable bladder (leading to fluid retention).
• Blues - anxiety and depression
• Rigidity - muscle and morning joint stiffness
• Owch - widespread and chronuic pain, as well as tender points (hyperalgeic points).

Other symptoms commonly include numbness/tingling sensations and sensitivity to sensory stimuli such as bright lights, odours, noises etc.

Question 24

How is Fibromyalgia investigated?

Answer 24

Fibromyalgia diagnosis is based on history (full social, personal, family and psychological history) and examination revealing widespread pain above and below the waist as well as the axial skeletal system, for at least three months. The presence of 11/18 tender points must be shown.

All laboratory investigations are likely to be normal. (ESR, TFT, FBC, RA, anti-CCP, ANA, VitD levels).

Question 25

What is the definition and epidemiology of Osteoarthritis?

Answer 25

Osteoarthritis is a disease in which the articular cartilage degenerates over time, causing pain and inflammation in the affected joint. It is the most common form of arthritis and is a major cause of impaired mobility. Around 10% of men and 18% of women >60 have symptomatic osteoarthritis.

Question 26

What are the risk factors of Osteoarthritis?

Answer 26

Idiopathic cause. However, risk factors include:
• Age >50
• Female gender
• Obesity
• Genetic factors (40-60% is thought to have a genetic component)
• Physical/manual occupation.

Question 27

[What is the pathophysiology of Oestoarthritis?]

Answer 27

Loss of chondrocyte cells (which normally produce collagen and proteoglycans for the hyaline cartilage) disrupts the normal repair mechanism. Overtime this leads to hyaline cartilage damage.

Certain cytokines (e.g. IL-2 and TNF-a) and protease enzymes are released in response to dead chondrocytes in the synovial fluid. This further triggers osteoarthritic changes through direct cartilage damage.

Eventually, cartilage damage exposes underlying bone. The friction of bone touching causes more inflammation and pain. Furthermore, the exposed bone is allowed to grow, causing subchondral bone growth. When growing outwards they are called osteophytes.

Question 28

What are the symptoms of Osteoarthritis?

Answer 28

Clinical features depend on the joint sites affected.
• Nodal OA or primarly generalised OA commonly affects post-menopausal women. There is hand pain, aching or stiffness for most days of the prior month. Heberden’s and Bouchard’s nodes are characteristic of nodal OA.
• Hip OA - hip pain for most days of the month.
• Knee OA - commonly presents in obese women >38 years of age.

In OA, joint pain is worse on movement, load bearing and at the end of the day. There is also periarticular tenderness over the site.

Joint stiffness occurs in the morning lasting for <30 minutes. There is reduced joint function (e.g. knee giving way) and joint instability.

Question 29

What are the examination features of Osteoarthritis?

Answer 29

There is commonly crepitus (audible or palpable creaking) of the joint on movement. There is also a lower range of movement, muscle wasting and often deformities such as Bouchard’s nodes (PIP) and Heberden’s nodes (DIP).

There may also be mild synovitis and effusion.

You may notice a limp/antalgic gait (gait that develops in order to avoid pain).

Question 30

How is Osteoarthritis investigated?

Answer 30

Bloods:
• ESR and CRP are normal
• RF and anti-CCP negative.

On X-Ray of joints there is:
• Loss of joint space
• Osteophytes
• Subchondral sclerosis
• Subchondral cysts.

MRI can also show early thinning of cartilage.

Question 31

What is the definition and epidemiology of RA?

Answer 31

Rheumatoid arthritis is a chronic systemic inflammatory disorder which primarily affects joints that are lined with synovium. It is the most common inflammatory arthritis affecting around 1% of the population.

Affects females 3:1 (before menopause, after menopause distribution is similar). RA can affect any age group, but the age of onset is often 20-40 years.

Question 32

What is the aetiology/risk factors for RA?

Answer 32

Unknown aetiology. Strong association between HLA-DR4 and HLA-DR1.

Risk factors include smoking, infection, diet and hormonal.

Question 33

What are the clinical features of RA?

Answer 33

Patients present with active symmetrical polyarthritis lasting >6 weeks. This causes joint pain and swelling. It usually affects the small joints of the hands and feet.

Patients also complain of morning stiffness that lasts >1 hour.

Onset of disease is relatively rapid (weeks to months) In early disease this usually causes swollen metacarpophalangeal (MCP), proximal interphalangeal (PIP), wrist or metatarsophalangeal (MTP) joints.

In later disease you may get boutonnière deformity (flexion of the PIP and hyperextension of the DIP) or swan neck deformity (hyperextension of the PIP and flexion of the DIP). Ulnar deviation of the fingers may also occur.

You may notice rheumatoid nodules in very active disease. In severe disease you may get vasculitis lesions, pleuritic chest pain and scleritis and/or uveitis. + Other extra-articular manifestations.

Question 34

What are the extra-articular manifestation of RA?

Answer 34

• Dry eyes and scleritis
• Pulmonary fibrosis
• Anaemia
• Rheumatoid nodules
• Drug-related ulcers of stomach and drug-related renal damage
• Osteoporosis

Question 35

How can RA be investigated?

Answer 35

↑Serum Rheumatoid Factor (RF) is present in up to 70% of patients. RF is an autoantibody against the Fc portion of IgG.

↑Serum anti-cyclic citrullinated peptide (anti-CCP) antibodies are also seen in up to 70% of patients, and is associated with smoking.

X-rays show erosions starting at the margins of joints.

Question 36

What is the definition and epidemiology of Giant Cell Arteritis?

Answer 36

GCA is the commonest form of vasculitis, typically affecting the temporal artery. It is an autoimmune disorder where exposure to an unknown environmental trigger causes a reaction against the arterial wall. It occurs almost exclusively in patients over 50 years of age, and affects females more than males (3:1). 50% of patients also have Polymyalgia Rheumatica.

Question 37

What are the clinical features of GCA?

Answer 37

GCA mainly affects the extra-cranial branches of the carotid artery (specifically the temporal artery) but can affect any branch of the aorta.

Presents as an abrupt onset headache, usually unilateral in the temporal area. Patients also complain of scalp pain, which can be worse when combing their hair.

50% of patients also have Polymyalgia Rheumatica and so have symptoms such as fever, fatigue, weight loss and muscle aching.

Patient may also have visual symptoms due to ophthalmic artery involvement (very serious complication), complaining of amaurosis fugax (transient loss of vision in one eye), blurring and diplopia, or partial or complete loss of vision.

Jaw and tongue claudication are uncommon symptoms.

Question 38

How is GCA investigated?

Answer 38

Blood tests:
• ↑ESR ≥50mm/hour (One of the diagnostic criteria), CRP is also elevated
• FBC may show normcocytic normochromic anaemia

A temporal artery biopsy may show a typical appearance of intermittent inflammation (skip lesions), or it even may be negative (20-30%).

An ultrasound may reveal thickening of the affected blood vessel wall (halo sign).

Question 39

What is the management of GCA?

Answer 39

Immediate administration of high-dose glucocorticoid after clinical suspicion of GCA. This is because visual loss occurs early in the course of the disease, and is irreversible. Glucocorticoid is essential in preventing further visual deterioration.

Treatment is then dependent on complications, but is essentially continuing glucocorticoids (prednisolone) until absence or reduction of clinical symptoms.

Bone protection such as bisphosphonate and calcium/vitamin D supplementation should be strongly considered.

Question 40

What is the definition and epidemiology of Gout?

Answer 40

Gout is an inflammatory arthritis which progresses from asymptomatic hyperuricaemia (elevated uric acid levels). The prevalence of gout in the UK is 1.4% and is increasing because of obesity and dietary factors. Affects males more than females 4:1.

Question 41

What is the aetiology of Gout?

Answer 41

Gout is precipitated by a state of hyperuricaemia. This can be due to a variety of factors including:
• Increased consumption of purines (dietary factors)
• Increased production of purines (dietary factors)
• Decreased clearance of uric acid - dehydration
• Obesity and diabetes
• Chemotherapy and radiation
• Genetic predisposition
• CKD
• Certain medications.

The uric acid combines with sodium to form monosodium urate crystals which are sharp crystals, that deposit in the joints and kidneys.

Question 42

What are the clinical features of Gout?

Answer 42

Most commonly affects the first metatarso-phalangeal joint (MTP) and causes Podagra (condition caused by gout at the first MTP). Other common sites includes the elbow, wrist, knee and ankle. 90% of gout attacks are monoarthritic.

The single peripheral joint becomes excruciatingly painful (often starting at night) and becomes red, hot and swollen. The pain becomes progressively worse over 6-12 hours. This is called acute gout. Chronic gout may also develop, which is seen by tophi.

Question 43

What are the investigations of Gout?

Answer 43

Joint aspiration and synovial fluid analysis can be done to provide a definitive diagnosis by demonstrating the presence of negatively birefringent crystals under polarised light microscopy.

Serum urate measurement is often elevated, and is a useful way to monitor the response to treatment.

Radiographs may show soft-tissue swellings.

Question 44

What is the definition and epidemiology of Psuedogout?

Answer 44

Pseudogout, also called calcium pyrophosphate disease is caused by the deposition of calcium pyrophosphate crystals. It is more common than gout affecting 7%. Affects people over the age of 40 and affects males and females equally.

Question 45

What are the clinical features of Pseudogout?

Answer 45

The patient may be asymptomatic but picked up on X-Ray.

Inflammation causes acute tender, red, hot, swollen joint (acute CPP). Affects like osteoarthritis - knee, wrist and ankle.

Patients that complain of pain and stiffness with long-term damage to joints (usually knees, wrists, hips and shoulders).

Question 46

How is Pseudogout investigated?

Answer 46

Joint aspiration and analysis will show white blood cells as well as positive birefringent rhomboid-shaped crystals.

Serum calcium or PTH may be elevated.

Ultrasound may show calcium deposits.

Blood tests show leucocytosis, and ↑CRP and ESR.