Fanconi anemia differential diagnosis: Difference between revisions

	Fanconi anemia Microchapters
Home
Patient Information
Overview
Historical Perspective
Classification
Pathophysiology
Causes
Differentiating Fanconi anemia from other Diseases
Epidemiology and Demographics
Risk Factors
Screening
Natural History, Complications and Prognosis
Diagnosis
Diagnostic Study of Choice
History and Symptoms
Physical Examination
Laboratory Findings
Electrocardiogram
X Ray
CT
MRI
Ultrasound
Other Imaging Findings
Other Diagnostic Studies
Treatment
Medical Therapy
Surgery
Primary Prevention
Secondary Prevention
Cost-Effectiveness of Therapy
Future or Investigational Therapies
Case Studies
Case #1
Fanconi anemia differential diagnosis On the Web
Most recent articles
Most cited articles
Review articles
CME Programs
Powerpoint slides
Images
American Roentgen Ray Society Images of Fanconi anemia differential diagnosis All Images X-rays Echo & Ultrasound CT Images MRI
Ongoing Trials at Clinical Trials.gov
US National Guidelines Clearinghouse
NICE Guidance
FDA on Fanconi anemia differential diagnosis
CDC on Fanconi anemia differential diagnosis
Fanconi anemia differential diagnosis in the news
Blogs on Fanconi anemia differential diagnosis
Directions to Hospitals Treating Fanconi anemia
Risk calculators and risk factors for Fanconi anemia differential diagnosis

VisualWikitext

Revision as of 15:57, 24 June 2018

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				Lab Findings	Imaging	Histopathology
Clinical manifestations			Pathophysiology	Para-clinical findings			Gold standard	Additional findings
Disease	Symptom	Physical exam		Blood profile	Anamalies	Histopathology
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		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		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

References

Template:WH Template:WS

@@ Line 18: / Line 18: @@
 |+
 |- style="background: #4479BA; color: #FFFFFF; text-align: center;"
-| colspan="7" rowspan="1" style="background: #4479BA; color: #FFFFFF; text-align: center;" |'''Clinical manifestations'''
+| colspan="3" rowspan="2" |'''Clinical manifestations'''
-! colspan="7" rowspan="2" style="background: #4479BA; color: #FFFFFF; text-align: center;" |Para-clinical findings
+| rowspan="3" |Pathophysiology
-| colspan="1" rowspan="4" style="background: #4479BA; color: #FFFFFF; text-align: center;" |'''Gold standard'''
+! colspan="3" style="background: #4479BA; color: #FFFFFF; text-align: center;" |Para-clinical findings
-! rowspan="4" style="background: #4479BA; color: #FFFFFF; text-align: center;" |Additional findings
+| colspan="1" rowspan="3" style="background: #4479BA; color: #FFFFFF; text-align: center;" |'''Gold standard'''
+! rowspan="3" style="background: #4479BA; color: #FFFFFF; text-align: center;" |Additional findings
 |-
-| colspan="4" rowspan="2" style="background: #4479BA; color: #FFFFFF; text-align: center;" |'''Symptoms'''
+! style="background: #4479BA; color: #FFFFFF; text-align: center;" |Lab Findings
-! colspan="3" rowspan="2" style="background: #4479BA; color: #FFFFFF; text-align: center;" |Physical examination
+! style="background: #4479BA; color: #FFFFFF; text-align: center;" |Imaging
+! rowspan="2" style="background: #4479BA; color: #FFFFFF; text-align: center;" |Histopathology
 |-
-! colspan="3" style="background: #4479BA; color: #FFFFFF; text-align: center;" |Lab Findings
+|Disease
-! colspan="3" style="background: #4479BA; color: #FFFFFF; text-align: center;" |Imaging
+! style="background: #4479BA; color: #FFFFFF; text-align: center;" |Symptom
-! rowspan="2" style="background: #4479BA; color: #FFFFFF; text-align: center;" |Histopathology
+! style="background: #4479BA; color: #FFFFFF; text-align: center;" |Physical exam
-|-
+! style="background: #4479BA; color: #FFFFFF; text-align: center;" |Blood profile
-! style="background: #4479BA; color: #FFFFFF; text-align: center;" |Symptom 1
+! style="background: #4479BA; color: #FFFFFF; text-align: center;" |Anamalies
-|
-! colspan="1" rowspan="1" style="background: #4479BA; color: #FFFFFF; text-align: center;" |Symptom 2
-! style="background: #4479BA; color: #FFFFFF; text-align: center;" |Symptom 3
-! style="background: #4479BA; color: #FFFFFF; text-align: center;" |Physical exam 1
-! colspan="1" rowspan="1" style="background: #4479BA; color: #FFFFFF; text-align: center;" |Physical exam 2
-! style="background: #4479BA; color: #FFFFFF; text-align: center;" |Physical exam 3
-! style="background: #4479BA; color: #FFFFFF; text-align: center;" |Lab 1
-! style="background: #4479BA; color: #FFFFFF; text-align: center;" |Lab 2
-! style="background: #4479BA; color: #FFFFFF; text-align: center;" |Lab 3
-! style="background: #4479BA; color: #FFFFFF; text-align: center;" |Imaging 1
-! style="background: #4479BA; color: #FFFFFF; text-align: center;" |Imaging 2
-! style="background: #4479BA; color: #FFFFFF; text-align: center;" |Imaging 3
 |-
+|Fanconi Anemia
 |Short stature, delicate features, upper limbs absent or hypoplastic thumbs, supernumerary, bifid clinodactyly
-|Fanconi Anemia
+infection, petechia, pallor
-|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,
-|Head – Microcephaly or hydrocephaly; birdlike face, mid-face hypoplasia, Sprengel's deformity of neck,
 Eyes- Microphthalmia, ptosis, epicanthal folds, strabismus
-|Complete blood count
-Peripheral blood smear
-Reticulocyte count
-Complete metabolic panel
-Prothrombin time/partial
-thromboplastin time (PT/PTT)
-Blood type and screen
-|Cytopenia,
-Bone marrow failure
-|
 |
-|Gastrointestinal anomalies – Atresias, imperforate anus, tracheoesophageal fistula, malrotation,
+|Anemia
+normocellular or hypercellular bone marrow
+|Gastrointestinal  Atresias, imperforate
+anus, TE fistula, malrotation,
 Kidney – Abnormal, ectopic, horseshoe, hypoplastic, or absent kidney; hydronephrosis
-|Cardiopulmonary anomalies – Congenital heart disease (patent ductus arteriosus, atrial or ventricular septal defects, coarctation, situs inversus)
 |
-|FA gene sequencing
+|FA gene
+sequencing
 |Incrreased chromosomal breakage in response to mitomycin C or diepoxybutane (quite sensitive but not entirely specific)
 |-
-| style="background: #F5F5F5; padding: 5px;" |recurrent infections due to neutropenia, mucosal hemorrhage or menorrhagia due to thrombocytopenia, or fatigue and cardiopulmonary findings associated with progressive anemia.
 | style="background: #DCDCDC; padding: 5px; text-align: center;" |Acquired Aplastic Anemia
-| style="background: #F5F5F5; padding: 5px;" |infections including bacterial and fungal in cases of severe neutropenia
+| style="background: #F5F5F5; padding: 5px;" |infections  mucosal hemorrhage menorrhagia
-| style="background: #F5F5F5; padding: 5px;" |Transient pancytopenia and bone marrow hypoplasia may be caused by a number of exposures including medications, chemicals, certain viral infections, and sepsis or other severe bacterial infections.
 | style="background: #F5F5F5; padding: 5px;" |especially pallor and petechiae.
-| style="background: #F5F5F5; padding: 5px;" |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
-| style="background: #F5F5F5; padding: 5px;" |
+|
-| style="background: #F5F5F5; padding: 5px;" |Complete blood count
+| style="background: #F5F5F5; padding: 5px;" |Anemia
+normocellular or hypercellular bone marrow
+| style="background: #F5F5F5; padding: 5px;" |Gastrointestinal  Atresias, imperforate
-Peripheral blood smear
+anus, TE fistula, malrotation,
-Reticulocyte count
+Kidney – Abnormal, ectopic, horseshoe, hypoplastic, or absent kidney; hydronephrosis
-Complete metabolic panel
-Prothrombin time/partial
-thromboplastin time (PT/PTT)
-Blood type and screen
-| style="background: #F5F5F5; padding: 5px;" |Serum chemistries, including electrolytes, liver function tests (including lactate dehydrogenase [LDH]), and renal function tests should be performed, Also serum B12 and Folate should be performed to exclude
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
 | style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |Bone marrow aspiration and Biopsy= hypocellular bone marrow in the absence of an abnormal infiltrate or marrow fibrosis.
+| style="background: #F5F5F5; padding: 5px;" |hypocellular bone
-| style="background: #F5F5F5; padding: 5px;" |typically a more rapid onset and progression of cytopenias; and a response to immunosuppressive therapy
+marrow
+| style="background: #F5F5F5; padding: 5px;" |rapid onset
 |-
+| style="background: #DCDCDC; padding: 5px; text-align: center;" |Paroxysmal nocturnal hemoglobinuria (PNH)
 | style="background: #F5F5F5; padding: 5px;" |Fatigue
@@ Line 112: / Line 76: @@
 ●Hemoglobinuria
-| style="background: #DCDCDC; padding: 5px; text-align: center;" |Paroxysmal nocturnal hemoglobinuria (PNH)
-| style="background: #F5F5F5; padding: 5px;" |Abdominal pain
+Abdominal pain
 ●Bone marrow suppression
 ●Erectile dysfunction
-| style="background: #F5F5F5; padding: 5px;" |Chest pain
+Chest pain
 ●Thrombosis
@@ Line 124: / Line 89: @@
 ●Renal insufficiency
 | style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
+|
-| style="background: #F5F5F5; padding: 5px;" |
 | style="background: #F5F5F5; padding: 5px;" |Anemia
-●Increased reticulocyte count
+normocellular or hypercellular bone marrow
-●Increased lactate dehydrogenase (LDH) and bilirubin
-●Decreased haptoglobin
-●Free serum hemoglobin with pink/red serum
-'''Bone Marrow''': PNH usually have a normocellular or hypercellular bone marrow with erythroid hyperplasia. Stainable iron is often absent
-| style="background: #F5F5F5; padding: 5px;" |hemolytic anemia (indirect hyperbiliribinemia)
- Intravascular hemolysis in PNH can lead to [[ARF]] and [[Chronic renal disease|CRD]].
-| style="background: #F5F5F5; padding: 5px;" |●Hypocellular, normocellular or hypercellular bone marrow, often with erythroid hyperplasia; erythroid dysplasia is not uncommon
 | style="background: #F5F5F5; padding: 5px;" |
+| style="background: #F5F5F5; padding: 5px;" |●Hypo/Hyper
+/Normo
-| style="background: #F5F5F5; padding: 5px;" |●Findings of iron deficiency may be seen in some patients due to excessive iron loss from hemoglobinuria and hemosiderinuria (eg, low iron, low ferritin, increased transferrin, absent bone marrow iron
+cellular,
-| style="background: #F5F5F5; padding: 5px;" |●Hemoglobinuria with pink/red urine, positive dipstick for heme, and negative sediment for red blood cells
+| style="background: #F5F5F5; padding: 5px;" |Flow cytometry
-●Negative direct antiglobulin (Coombs) test (DAT)
-| style="background: #F5F5F5; padding: 5px;" |●Hypocellular, normocellular or hypercellular bone marrow, often with erythroid hyperplasia; erythroid dysplasia is not uncommon
-| style="background: #F5F5F5; padding: 5px;" |'''FLAER''': Flow cytometry detect (GPI) anchored proteins, which are reduced or absent on blood cells in PNH.
-Acquired mutations in the ''PIGA'' gene result in the dominance of a hematopoietic progenitor cell clone lacking glycosylphosphatidylinositol (GPI) anchors
 | style="background: #F5F5F5; padding: 5px;" |
 |-
-| style="background: #F5F5F5; padding: 5px;" |
 | style="background: #DCDCDC; padding: 5px; text-align: center;" |Other inherited bone marrow failure syndromes
 (Dyskeratosis congenita and other short telomere syndromes)
 | style="background: #F5F5F5; padding: 5px;" |'''Bone marrow failure'''
 Classic mucocutaneous and additional dermatologic findings
@@ Line 181: / Line 130: @@
 •Microcephaly
-| style="background: #F5F5F5; padding: 5px;" |●Pulmonary disease (pulmonary fibrosis)
+Pulmonary disease (pulmonary fibrosis)
 ●Endocrine/Growth/Urologic
@@ Line 211: / Line 160: @@
 ●Cancer
+|
+| style="background: #F5F5F5; padding: 5px;" |Reticular dysgenesis
 | style="background: #F5F5F5; padding: 5px;" |
 | style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |Reticular dysgenesis (RD) is a type of severe combined immunodeficiency caused by mutations in the ''AK2 ''gene that may also be associated with bone marrow aplasia,
+| style="background: #F5F5F5; padding: 5px;" |Flow cytometry
+| style="background: #F5F5F5; padding: 5px;" | - chromosomal breakage test.
-unlike FA, patients with RD develop bone marrow aplasia in infancy associated with sensorineural hearing loss and severe adaptive immune dysfunction
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |negative chromosomal breakage test.
-|- style="background: #4479BA; color: #FFFFFF; text-align: center;"
-!Symptom 1
-!Diseases
-! colspan="1" rowspan="1" |Symptom 2
-!Symptom 3
-!Physical exam 1
-! colspan="1" rowspan="1" |Physical exam 2
-!Physical exam 3
-!Lab 1
-!Lab 2
-!Lab 3
-!Imaging 1
-!Imaging 2
-!Imaging 3
-!Histopathology
-|'''Gold standard'''
-!Additional findings
 |-
-| style="background: #F5F5F5; padding: 5px;" |
 | style="background: #DCDCDC; padding: 5px; text-align: center;" |Drug-induced or infection-associated pancytopenia
 | style="background: #F5F5F5; padding: 5px;" |
 | style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
+|
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
 | style="background: #F5F5F5; padding: 5px;" |
 | style="background: #F5F5F5; padding: 5px;" |
@@ Line 259: / Line 177: @@
 | style="background: #F5F5F5; padding: 5px;" |
 |-
-| style="background: #F5F5F5; padding: 5px;" |Like FA, these rare chromosomal instability syndromes are associated with multiple congenital anomalies, often including microcephaly, short stature, and increased risk of malignancy. Also like FA, t.
+| style="background: #DCDCDC; padding: 5px; text-align: center;" |Rare syndromes,
-| style="background: #DCDCDC; padding: 5px; text-align: center;" |Rare chromosomal breakage syndromes, Nijmegen breakage syndrome (''NBS''), Bloom syndrome (''BLM''), ataxia telangiectasia (''ATM''), LIG4 syndrome (''LIG4''), NHEJ1 deficiency (''NHEJ1''), Seckel syndrome ''(ATR)'','' ''and the cohesinopathies Roberts syndrome (''ESCO2'') and Warsaw breakage syndrome (''DDX11'').
+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'').
+| style="background: #F5F5F5; padding: 5px;" |microcephaly, short stature increased
+malignancy
 | style="background: #F5F5F5; padding: 5px;" |
+|
+| style="background: #F5F5F5; padding: 5px;" |no specific findings
+| style="background: #F5F5F5; padding: 5px;" |Gastrointestinal  Atresias, imperforate
+anus, TE fistula, malrotation,
+Kidney – Abnormal, ectopic, horseshoe, hypoplastic, or absent kidney; hydronephrosis
 | style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
+| style="background: #F5F5F5; padding: 5px;" |abnormal chromosomal breakage test
-| style="background: #F5F5F5; padding: 5px;" |
+| style="background: #F5F5F5; padding: 5px;" |No bone
-| style="background: #F5F5F5; padding: 5px;" |
+marrow
-| style="background: #F5F5F5; padding: 5px;" |compared to FA, these conditions show subtle differences in the associated congenital anomalies, the spectrum of associated malignancies, and the specific abnormalities seen within chromosomal breakage testing (eg, increased chromosome 7 and 14 abnormalities in NBS, railroading figures in cohesinopathies).
-| style="background: #F5F5F5; padding: 5px;" |
+failure
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |these syndromes will often cause an abnormal chromosomal breakage tes
-| style="background: #F5F5F5; padding: 5px;" |patients with NBS do not typically exhibit bone marrow failure except in the setting of evolving malignancy.
 |-
+| style="background: #DCDCDC; padding: 5px; text-align: center;" |De novo myelodysplastic syndrome (MDS)
 | style="background: #F5F5F5; padding: 5px;" |MDS can arise de novo or secondary to another bone marrow disorder;
-| style="background: #DCDCDC; padding: 5px; text-align: center;" |De novo myelodysplastic syndrome (MDS)
-| style="background: #F5F5F5; padding: 5px;" |many patients with FA develop secondary MDS in child/young adults.
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |de novo MDS can cause bone marrow failure
-| style="background: #F5F5F5; padding: 5px;" |variable cytopenias, multilineage dysplasia, cytogenetic abnormalities, and increased blasts
-| style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |
 | style="background: #F5F5F5; padding: 5px;" |
+|
+| style="background: #F5F5F5; padding: 5px;" |bone marrow failure
 | style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |, individuals with MDS in whom FA is being considered should have chromosomal breakage tests performed on skin fibroblasts rather than hematopoietic cells, because bone marrow cytogenetic abnormalities associated with MDS clones may skew chromosomal breakage results performed on lymphocyte
+| style="background: #F5F5F5; padding: 5px;" |Positive
+chromosomal breakage tests
 | style="background: #F5F5F5; padding: 5px;" |
-| style="background: #F5F5F5; padding: 5px;" |Unlike FA or FA with secondary MDS, de novo MDS is not associated with congenital anomalies, an abnormal chromosome breakage test, or FA mutations
+| style="background: #F5F5F5; padding: 5px;" |Negitive
+chromosomal breakage tests
 |}