Fanconi anemia differential diagnosis: Difference between revisions
Amar Morani (talk | contribs) mNo edit summary |
Amar Morani (talk | contribs) mNo edit summary |
||
Line 59: | Line 59: | ||
| style="background: #F5F5F5; padding: 5px;" |especially pallor and petechiae. | | style="background: #F5F5F5; padding: 5px;" |especially pallor and petechiae. | ||
The liver, spleen, and lymph nodes are typically enlarged in AA, if its enlarged it may suggest alternative diagnosis | The liver, spleen, and lymph nodes are typically enlarged in AA, if its enlarged it may suggest alternative diagnosis | ||
| | |cause remains | ||
obscure in most cases. | |||
Immune system abnormalitis and genetic predisposition | |||
may play role | |||
| style="background: #F5F5F5; padding: 5px;" |Anemia | | style="background: #F5F5F5; padding: 5px;" |Anemia | ||
normocellular or hypercellular bone marrow | normocellular or hypercellular bone marrow |
Revision as of 16:35, 24 June 2018
Fanconi anemia Microchapters |
Diagnosis |
---|
Treatment |
Case Studies |
Fanconi anemia differential diagnosis On the Web |
American Roentgen Ray Society Images of Fanconi anemia differential diagnosis |
Risk calculators and risk factors for Fanconi anemia differential diagnosis |
Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief:
Overview
Fanconi Anemia must be differentiated from Aplastic Anemia, Paraoxysomal Nocturnal Hemoglobinuria, and Chromosomal breakage syndrome and Hereditary Bone marrow failure syndrome (Dyskeratosis congenita and other short telomere syndromes).
Differentiating X from other Diseases
- Fanconi Anemia must be differentiated from other diseases that cause Pancytopenia, Congenital anomalies, and associated with malignancy such as Aplastic Anemia, Rare chromosomal breakage syndrome and inherited bone marrow failure.
- As Fanconi Anemia resembles with variety of other diseases that causes pancytopenia.
- Must be differentiated on basis on congenital anomalies and chromosomal breakage test.
Preferred Table
Clinical manifestations | Pathophysiology | Para-clinical findings | Gold standard | Additional findings | ||||
---|---|---|---|---|---|---|---|---|
Lab Findings | Imaging | Histopathology | ||||||
Disease | Symptom | Physical exam | Blood profile | Anamalies | ||||
Fanconi Anemia | Short stature, delicate features, upper limbs absent or hypoplastic thumbs, supernumerary, bifid clinodactyly
infection, petechia, pallor |
Skin – Generalized hyperpigmentation; hypopigmented areas; large freckles, café-au-lait spots
Head – Microcephaly or hydrocephaly; birdlike face, mid-face hypoplasia, Sprengel's deformity of neck, Eyes- Microphthalmia, ptosis, epicanthal folds, strabismus |
Inherited defect in DNA Repair causes loss of HSC that leads
to bone marrow failure. |
Anemia
normocellular or hypercellular bone marrow |
Gastrointestinal Atresias, imperforate
anus, TE fistula, malrotation, Kidney – Abnormal, ectopic, horseshoe, hypoplastic, or absent kidney; hydronephrosis |
FA gene
sequencing |
Incrreased chromosomal breakage in response to mitomycin C or diepoxybutane (quite sensitive but not entirely specific) | |
Acquired Aplastic Anemia | infections mucosal hemorrhage menorrhagia | especially pallor and petechiae.
The liver, spleen, and lymph nodes are typically enlarged in AA, if its enlarged it may suggest alternative diagnosis |
cause remains
obscure in most cases. Immune system abnormalitis and genetic predisposition may play role |
Anemia
normocellular or hypercellular bone marrow |
Gastrointestinal Atresias, imperforate
anus, TE fistula, malrotation, Kidney – Abnormal, ectopic, horseshoe, hypoplastic, or absent kidney; hydronephrosis |
hypocellular bone
marrow |
rapid onset | |
Paroxysmal nocturnal hemoglobinuria (PNH) | Fatigue
●Dyspnea ●Hemoglobinuria Abdominal pain ●Bone marrow suppression ●Erectile dysfunction Chest pain ●Thrombosis ●Renal insufficiency |
Anemia
normocellular or hypercellular bone marrow |
●Hypo/Hyper
/Normo cellular, |
Flow cytometry | ||||
Other inherited bone marrow failure syndromes
(Dyskeratosis congenita and other short telomere syndromes) |
Bone marrow failure
Classic mucocutaneous and additional dermatologic findings •Skin dyspigmentation •Nail irregularities •Leukoplakia •Premature graying/hair loss •Hyperhidrosis – 15 percent Ophthalmologic/Epiphora (excessive tearing/lacrimal duct stenosis) ●Neurologic/Cognitive •Developmental delay •Ataxia/cerebellar hypoplasia – approximately •Microcephaly Pulmonary disease (pulmonary fibrosis) ●Endocrine/Growth/Urologic features •Short stature •Intrauterine growth retardation •Hypogonadism/Undescended testes •Urethral stricture/phimosis •Osteoporosis and related complications |
Unlike Fanconi anemia, individuals with DC do not appear to have impaired fertility
●Dental manifestations (caries) ●Gastroenterologic/Hepatologic manifestations •Esophageal strictures •Liver disease (cirrhosis, fibrosis) or gastroenteropathy ●Cancer |
Reticular dysgenesis | Flow cytometry | - chromosomal breakage test. | |||
Drug-induced or infection-associated pancytopenia | ||||||||
Rare syndromes,
Nijmegen breakage syndrome (NBS), Bloom syndrome (BLM), ataxia telangiectasia (ATM), LIG4 syndrome (LIG4), NHEJ1 deficiency (NHEJ1), Seckel syndrome (ATR), cohesinopathies Roberts syndrome (ESCO2) Warsaw breakage syndrome (DDX11). |
microcephaly, short stature increased
malignancy |
no specific findings | Gastrointestinal Atresias, imperforate
anus, TE fistula, malrotation, Kidney – Abnormal, ectopic, horseshoe, hypoplastic, or absent kidney; hydronephrosis |
abnormal chromosomal breakage test | No bone
marrow failure | |||
De novo myelodysplastic syndrome (MDS) | MDS can arise de novo or secondary to another bone marrow disorder; | bone marrow failure | Positive
chromosomal breakage tests |
Negitive
chromosomal breakage tests |