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Transthyretin amyloidosis

Last revised by Joachim Feger on 27 Apr 2024

Citation, DOI, disclosures and article data

Citation:

Feger J, Sharma R, Transthyretin amyloidosis. Reference article, Radiopaedia.org (Accessed on 31 May 2024) https://doi.org/10.53347/rID-187001

DOI:

https://doi.org/10.53347/rID-187001

Permalink:

https://radiopaedia.org/articles/187001

rID:

187001

Article created:

31 Mar 2024, Joachim Feger ◉

Disclosures:

At the time the article was created Joachim Feger had no financial relationships to ineligible companies to disclose.

View Joachim Feger's current disclosures

Last revised:

27 Apr 2024, Joachim Feger ◉

Disclosures:

At the time the article was last revised Joachim Feger had no financial relationships to ineligible companies to disclose.

View Joachim Feger's current disclosures

Revisions:

7 times, by 2 contributors - see full revision history and disclosures

Systems:

Cardiac, Musculoskeletal, Gastrointestinal

Tags:

amyloidosis

Synonyms:

Transthyretin-related amyloidosis
TTR amyloidosis
Wild-type ATTR amyloidosis
Variant ATTR amyloidosis
Senile amyloidosis
Hereditary ATTR amyloidosis
Familial ATTR amyloidosis
ATTRwt amyloidosis
ATTRv amyloidosis
Mutant ATTR amyloidosis
ATTR amyloidosis
Familial amyloid polyneuropathy (FAP)
Familial amyloid polyneuropathy

Transthyretin (ATTR) amyloidosis is a form of systemic amyloidosis characterized by the misfolding, aggregation and deposition of transthyretin-related (TTR) protein in various organs ^1-6. This can occur in the following two forms namely in the setting of a genetically normal transthyretin-related protein also referred to as wild-type transthyretin (ATTRwt) amyloidosis, and in the context of an amyloidogenic mutation of transthyretin, which is then termed variant transthyretin (ATTRv) amyloidosis ^1-5.

The genetically normal form or wild type mainly affects the heart and soft tissues. For the hereditary or variant forms cardiomyopathy-predominant, polyneuropathy-predominant and mixed phenotypes are distinguished ^1-5 and additionally a type with occuloleptomeningeal involvement ^5,6.

The true incidence and prevalence of ATTR amyloidosis and transthyretin amyloid cardiomyopathy are currently unknown due to population-based and regional variations of the genetic variant, and also due to low awareness and fragmented knowledge of the disease, resulting in underdiagnosis due to phenotypic heterogeneity and overlap with other clinical conditions ^1-9.

Wild-type transthyretin amyloidosis has been increasingly recognized as a cause of heart failure in the elderly ^1-9. Misfolding and aggregation seem to increase with age ^10-12 with autopsy series indicating TTR amyloid deposits in up to 25% of patients over the age of 80 years ^10-12 (however, not all of them to a clinically manifesting degree). The median age at the time of diagnosis is approximately 75 years and men are far more commonly affected ^1-4.

Variant transthyretin-related is the most common form of hereditary amyloidosis with variable phenotypes and varying ages at the onset of the disease ^1-4. The most common mutation is p.Val50Met (formerly Val30Met) ^3,4 with an early onset phenotype mainly seen in Portuguese, Brazilian, Japanese and Swedish populations and a late onset phenotype found worldwide. Other common variants are seen in North America and Western Africa in African-American populations in the Irish and other European regions such as Denmark and Italy ^4,5.

Associations

Transthyretin amyloidosis might be associated with the following clinical conditions ^1-6:

heart failure with preserved ejection fraction (6-30%) ^4,14
aortic stenosis – low-flow-low-gradient (up to 16%) ¹⁵
peripheral neuropathy ¹⁶
monoclonal gammopathy of undetermined significance
wild-type ATTR ^17-19:
- carpal tunnel syndrome
- lumbar spinal stenosis
- spontaneous distal biceps tendon rupture
- trigger finger
variant ATTR ^16,20:
- polyneuropathy
- autonomic dysfunction
- gastrointestinal problems
- vitreous opacities
- leptomeningeal involvement

Diagnosis

The diagnosis can be established histopathologically and consecutive amyloid typing (e.g. by determination of precursor protein by mass spectrometry). This can be done by tissue biopsy of the affected organ (e.g. the heart or peripheral nerves) or at other sites including the gastrointestinal mucosa, abdominal fat pad and salivary glands ^3,12,13,16.

Alternatively, the diagnosis can be established noninvasively in the following context ^12,13,21:

positive bone scintigraphy (^99mTc-PYP, ^99mTc-DPD, , ^99mTc-HMDP) with a Perugini grade 2 or 3
characteristic findings on echocardiography or cardiac magnetic resonance
negative serum-free light chains as well as serum and urine immunofixation tests

In addition, genetic testing is part of the diagnostic work-up ¹².

Clinical presentation

Due to its phenotypic heterogeneity symptoms are often variable and unspecific leading to a delay in diagnosis ^3-5.

In wild-type transthyretin-related amyloidosis, presenting symptoms are often cardiac in origin, including fatigue, dizziness, dyspnea and exercise intolerance ¹.

In variant transthyretin-related amyloidosis, a cardiac and a neurological phenotype are distinguished, with the neurological phenotype showing symptoms of peripheral neuropathy and autonomic dysfunction, the latter potentially causing orthostatic dysfunction and syncope ^4,12,13.

Other extracardiac symptoms include musculoskeletal or gastrointestinal symptoms, erectile dysfunction or unexplained weight loss ^1-3,12,13.

In addition to the clinical symptoms the following tests might be abnormal ^2-5,12,13:

NT-proBNP or troponin levels might be elevated, increase over time and are thus included in staging systems ^2-5
ECG might show decreased limb QRS voltage (≤5 mV)
abnormal nerve conduction studies and autonomic testing

Complications

Complications include the following ^3-5,13:

Pathology

Transthyretin-related amyloidosis is characterized by misfolding, aggregation and deposition of transthyretin-related protein as insoluble amyloid fibrils in the extracellular space of various organs including the heart, vasculature, the peripheral and autonomic nervous system, the soft tissues and gastrointestinal tract ^1-4. The amyloid fibrils are formed by the transport protein transthyretin (TTR) after dissociation of its tetrameric form into monomers and subsequent misfolding, either as a result of favorable conditions like oxidative stress or aging or in the context of an amyloidogenic mutation facilitating the process ^3,5 Transthyretin is mainly synthesized in the liver and to a lesser extent in the choroid plexus and by retinal pigment epithelial cells ^3,5.

Subtypes

Transthyretin-related amyloidosis features the following subtypes ¹:

wild-type (ATTRwt): genetically normal protein with an intrinsic tendency to form amyloid under certain conditions
variant from (ATTRv): amyloidogenic mutation promoting the formation of amyloid fibrils

Microscopic appearance

Amyloidosis is confirmed histopathologically by Congo red positivity of the extracellular amyloid deposits showing their fibrillar ultrastructure associated with apple green birefringence under polarized light ^1-5.

Immunophenotype

Transthyretin-related protein can be detected immunohistochemically in affected tissues using an anti-transthyretin antibody ¹⁸. Immunohistochemistry and related methods such as immunofluorescence and immunoelectron microscopy are considered alternative methods to mass spectrometry, they are however less sensitive and less specific ¹.

Genetics

Genetic sequencing and counseling are considered an essential part of the evaluation of ATTR amyloidosis for the following reasons ^1,12:

differentiating wild-type ATTR from variant ATTR
identification of relatives at risk
potentially influence of treatment strategies and prognosis

The tetrameric serum protein transthyretin is encoded by the TTR gene found on chromosome 18q12.1 and spanning four exons ⁴. More than 140 different mutations are known ⁴ with the more common forms causing variant ATTR being p.Val142Ile (formerly Val122) common in African-Americans, p.Val50Met (formerly Val30) common among Portuguese, Japanese and Swedish populations) and p.Thr80Ala (formerly Thr60Ala) common among the Irish people ^4,12.

Radiographic features

Imaging features of cardiac amyloidosis in general include the following ^12,13,22-24:

unexplained increased wall thickness of the following structures:
- left ventricular myocardium: often asymmetric
- right ventricular free wall
- interatrial septum and right atrial wall
- atrioventricular valves
biatrial enlargement

Additionally ^22-24:

Echocardiography

Echocardiography serves as a first-line imaging tool in the evaluation of cardiac involvement of amyloidosis. Echocardiographic criteria for cardiac amyloidosis in general include an increased wall thickness (≥12 mm) and other characteristic features such as ^12,13,22:

diastolic dysfunction
decreased tissue Doppler s’, e’ and a’ wave velocities (<5 cm/s)
decreased global longitudinal left ventricular strain with apical sparing ²²

Other common features include a ‘speckled pattern’ or ‘granular sparkling’ of the myocardium as well as biatrial enlargement ^2,13.

MRI

Cardiac MRI usually shows a significantly increased left ventricular mass, diffusely increased native T1 and very high ECV values on myocardial mapping and a variably diffuse to transmural non-ischemic late enhancement pattern as well as abnormal blood pool gadolinium kinetics ^12,13.

Signal characteristics

IRGE/PSIR: often diffuse late enhancement with right ventricular involvement ²⁵
T1 mapping: increased
ECV: markedly increased (often ≥50%) ^12,13

It is worth mentioning that a reliable differentiation between ATTR and AL on cardiac MRI is not possible ^12,13,22,23, still, MRI features favoring ATTR amyloidosis over AL include ^24,25:

asymmetrical wall thickening
high native T1 mapping values but lower than in AL amyloidosis
very high extracellular volume values >50%
high left and right ventricular wall thickness
high left ventricular mass >100 g/m²
late gadolinium enhancement is often more diffuse with right ventricular involvement and a QALE score >13

Nuclear medicine

Bone scintigraphy with Perugini grading is usually positive in the setting of cardiac ATTR-amyloidosis with a Perugini grade of 2 or 3, pointing to ATTR amyloidosis ^12,13,22.

However, in a significant percentage (>10%) of patients with AL amyloidosis bone scintigraphy has been also reported to be positive as well as in different other forms of amyloidosis ^7,8. Also, bone scintigraphy can be falsely positive in recent myocardial infarction (< 4 weeks), hydroxychloroquine cardiac toxicity as well as valvular or annular calcifications ¹³.

In addition, it can be negative in some ATTRv mutations ¹³.

Radiology report

The radiology report should include a description of the following:

morphology and functional analysis
wall motion abnormalities
left ventricular wall thickness
abnormal strain patterns (if measured)
valvular thickening and atrial enlargement (if present)

MRI

myocardial tissue properties including:
- presence, pattern and distribution of late gadolinium enhancement
- alteration of blood-pool gadolinium kinetics
- abnormal T1 and T2 mapping and ECV values (if performed)

Treatment and prognosis

Management includes guideline-directed therapy of cardiovascular symptoms, prevention and treatment of complications, new targeted therapeutic options aimed at preventing the dissociation of TTR molecules into amyloidogenic fragments by stabilizing their circulating forms (stabilizing molecules) and interfering with their production (genetic silencers) as well as supportive measures ^5,12,13.

The targeted therapy regimen depends mainly on the ATTR subtype (hereditary or wild type) and thus on the organ involvement of the disease, i.e. the presence of cardiomyopathy or polyneuropathy or both ⁷ and currently includes the following agents ^12,13:

TTR tetramer stabilizers: tafamidis, duflunisal, acoramidis
- in the setting of cardiomyopathy
gene silencers: partisiran, inotersen
- in the setting of polyneuropathy

Liver transplantation was the main treatment option in variant ATTR before the introduction of stabilizing and genetic silencing agents ^1,6.

The prognosis of transthyretin-related amyloidosis varies with the subtype, mutation and phenotype, the time of diagnosis as well as the presence of complications ranging from less than 3 years in patients with cardiomyopathy-predominant phenotypes up to 8 or 10 years in polyneuropathy-predominant variants and approximately 5 years in the setting of wild-type cardiac amyloidosis ^2,5.

The prognosis of transthyretin amyloidosis is generally better than in light chain amyloidosis, especially when the heart is involved ^6,12. The extent of late gadolinium enhancement and extracellular volume are considered predictors in cardiac amyloidosis ^23,26.

History and etymology

The term amyloid was first used for medical purposes by Rudolf Virchow in 1854 initially considering amyloid starch-based extracellular deposits ^27-29.

Senile amyloidosis was first reported by the Czech physician and pathologist Isidora Soyka in 1876 ^7,30. Hereditary ATTR amyloidosis was first reported in Portugal by the Portuguese neurologist Corino Andrade in 1952 and later in Japan and Sweden ^28,31-33.

Differential diagnosis

The main differential diagnosis of ATTR amyloidosis includes the following ^2,12:

light chain amyloidosis
other infiltrative cardiomyopathies such as Fabry disease
hypertensive heart disease
aortic stenosis
hypertrophic cardiomyopathy
chronic inflammatory demyelinating polyneuropathy
diabetic polyneuropathy
peripheral polyneuropathies
motor neuron disease

Practical points

ATTRwt has been considered a cardiac disease, whereas ATTRv has neuro-predominant and cardiac-predominant variants ³
on cardiac MRI, PSIR is an option to better deal with the difficulties of nulling myocardium ²⁶
the abdominal fat pad offers a rather low sensitivity as a biopsy site for ATTR amyloidosis (~45% in ATTRv and ~15% ATTRwt)
alternative biopsy sites for suspected ATTR are the labial salivary gland or the sural nerve, the latter, especially in the setting of polyneuropathy ²⁵
variant (hereditary) forms should undergo regular neurological as well as ophthalmological evaluations ¹³
follow-up should include yearly echocardiography or cardiac MRI ¹³

References

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