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Anophthalmia and Microphthalmia
Journal Pre-proof Anophthalmia and Microphthalmia Beryl R. Benacerraf, MD, Bryann S. Bromley, MD, Angie C. Jelin, MD PII:
S0002-9378(19)31018-X
DOI:
https://doi.org/10.1016/j.ajog.2019.08.016
Reference:
YMOB 12838
To appear in:
American Journal of Obstetrics and Gynecology
Please cite this article as: Benacerraf BR, Bromley BS, Jelin AC, Anophthalmia and Microphthalmia, American Journal of Obstetrics and Gynecology (2019), doi: https://doi.org/10.1016/j.ajog.2019.08.016. This is a PDF file of an article that has undergone enhancements after acceptance, such as the addition of a cover page and metadata, and formatting for readability, but it is not yet the definitive version of record. This version will undergo additional copyediting, typesetting and review before it is published in its final form, but we are providing this version to give early visibility of the article. Please note that, during the production process, errors may be discovered which could affect the content, and all legal disclaimers that apply to the journal pertain. © 2019 Published by Elsevier Inc.
SMFM Fetal Anomalies Consult Series #1: Facial Anomalies smfm.org 1
Anophthalmia and Microphthalmia
2
Beryl R. Benacerraf, MD; Bryann S. Bromley, MD; Angie C. Jelin, MD
3 4
Introduction
5
Anophthalmia and microphthalmia are characterized by the complete or almost complete lack of
6
the primary optic vesicle, resulting in an absent or very small malformed orbital globe.
7 8
Definition
9
Anophthalmia is the complete absence of the orbital globe. Microphthalmia refers to a small
10
typically malformed orbital globe. These abnormalities can be unilateral or bilateral. The birth
11
prevalence of these two malformations combined is approximately 1 per 10,000 births (1).
12 13
Ultrasound Findings
14
The fetal orbits are typically detectable by 11–12 weeks’ gestation, and the lens is seen as a thin,
15
walled circle within each orbit by 13–14 weeks gestation (2). The diagnosis of anophthalmia or
16
microphthalmia is typically a subjective one, although orbital measurements at each gestational
17
age are available (3). The coronal view of the fetal face is the best way to evaluate the orbits.
18
This view can show the size and shape of the orbits, their positioning on the fetal face, spacing
19
between the two orbits, and associated facial abnormalities. The sagittal view of each orbit is
20
also helpful when measuring the size of the orbit. The lens is seen as a small, thin-walled,
21
circular structure and is normally visible in the anterior aspect of the globe in both the axial and
22
sagittal views. The hyaloid artery is visible traversing the middle of the eye from anterior to
23
posterior usually by 14 weeks and should disappear by 29 weeks (4). Most often, the detection of
1
SMFM Fetal Anomalies Consult Series #1: Facial Anomalies smfm.org 24
these rare but severe ocular anomalies is made because other fetal anomalies are present and the
25
orbital findings are part of a syndrome. Orbital defects are rarely discovered prenatally as
26
isolated findings(see Figure 1).
27 28
Associated Abnormalities
29
The associated anomalies vary with the fetal syndrome involved; therefore, it is crucial to
30
perform a thorough sonographic anatomic evaluation. Triploidy and trisomies 9 and 13 are
31
among the aneuploidies most likely to feature microphthalmia. Triploidy has early asymmetric
32
fetal growth restriction associated with anomalies of the heart, brain, and face (hypertelorism).
33
Trisomy 13 is associated with midline facial and brain defects as well as cardiac anomalies and
34
polydactyly. Trisomy 9 results in early pregnancy loss; survival generally only occurs in mosaic
35
cases. Features of mosaic trisomy 9 include abnormalities of the heart, face, and skull.
36
Nonsyndromic conditions that can feature microphthalmia include holoprosencephaly spectrum,
37
congenital viral infections (particularly rubella), and CHARGE association (Coloboma, Heart
38
defects, Atresia choanae (choanal atresia), growth Restriction, Genital anomalies, and Ear
39
anomalies). Other syndromes associated with eye anomalies include Aicardi syndrome (female
40
fetus, arachnoid cyst); Fraser syndrome (genitourinary and tracheal anomalies); Fryns syndrome
41
(congenital diaphragmatic hernia); Goldenhar syndrome (ear tags, cleft lip and/or palate,
42
asymmetry of face); Gorlin syndrome (ventriculomegaly); Lenz syndrome (microcephaly);
43
Walker-Warburg syndrome (lissencephaly, ventriculomegaly, cataracts); fetal alcohol syndrome;
44
and others (5).
45 46
Differential Diagnosis
2
SMFM Fetal Anomalies Consult Series #1: Facial Anomalies smfm.org 47
Anomalies of the fetal eye may be bilateral or unilateral and asymmetrical. Anophthalmia and
48
microphthalmia refer to the size of the globe and orbit. Congenital cataracts should not be
49
confused with microphthalmia, although both conditions may be present in the same fetus. The
50
orbit may be distorted by masses such as intracranial teratomas (associated with intracranial
51
component), gliomas (usually medial aspect of orbit), or retinoblastomas (rarely seen in utero).
52 53
Genetic Evaluation
54
Diagnostic testing (amniocentesis or chorionic villus sampling) with chromosomal microarray
55
analysis (CMA) should be offered when anophthalmia is detected. If screening or other
56
ultrasound features are suggestive of a common aneuploidy, it is reasonable to initially perform
57
karyotype or fluorescence in situ hybridization, with reflex to CMA if these test results are
58
normal. Many syndromes are associated with anophthalmia; they can be sporadic, autosomal
59
dominant, autosomal recessive, or X-linked. If there are additional anomalies, consanguinity, or
60
a family history of a specific condition, gene panel testing or exome sequencing may be useful,
61
as CMA does not detect single-gene (Mendelian) disorders. If exome sequencing is pursued,
62
appropriate pretest and posttest genetic counseling by a provider experienced in the complexities
63
of genomic sequencing is recommended (6). Maternal infections (rubella), vitamin A deficiency,
64
and teratogenic exposures (thalidomide) have also been associated with anophthalmia; therefore,
65
obtaining a history of maternal exposures and a family history is important. After appropriate
66
counseling, cell-free DNA screening is an option for patients who decline diagnostic evaluation
67
if a common aneuploidy is suspected.
68 69
3
SMFM Fetal Anomalies Consult Series #1: Facial Anomalies smfm.org 70
Pregnancy and Delivery Management
71
A detailed ultrasound examination should be performed and should include comprehensive
72
imaging of the intracranial structures (e.g., a neurosonogram) and the fetal heart. A fetal
73
echocardiogram, as well as fetal magnetic resonance imaging to assess for intracranial
74
abnormalities, should be considered. Referrals to pediatric ophthalmology, craniofacial clinic,
75
plastic surgery, or other subspecialty services should be based on additional sonographic
76
findings. Pregnancy termination is an option that should be discussed with all patients in whom a
77
fetal anomaly is detected. Shared patient decision-making requires a thorough evaluation and
78
multidisciplinary counseling regarding prognosis. The specific finding of anophthalmia or
79
microphthalmia does not generally affect delivery management, although delivery at a tertiary
80
care center with pediatric genetic, craniofacial, and ophthalmology consultation should be
81
considered, as appropriate for the clinical findings.
82 83
Prognosis
84
The prognosis is variable and dependent upon the severity, associated anomalies, and underlying
85
genetic etiology. Unilateral microphthalmia can have a favorable prognosis other than possible
86
blindness in the affected eye. Mild to moderate microphthalmia can be managed with
87
conformers, whereas severe cases may require surgical remodeling. Bilateral microphthalmia is
88
often associated with intellectual disability, and vision is dependent upon retinal development.
89
Reported cases of anophthalmia typically represent severe microphthalmia, as true, primary
90
anophthalmia is rarely compatible with life secondary to associated cerebral anomalies.
91 92
Summary
4
SMFM Fetal Anomalies Consult Series #1: Facial Anomalies smfm.org 93
Microphthalmia is a rare abnormality of the eye that generally occurs due to a genetic syndrome,
94
maternal infection, teratogenic exposure, or vitamin deficiency. Diagnostic testing is
95
recommended with CMA and/or molecular genetic testing based on associated anomalies.
96
Prognostic counseling is dependent on the severity of microphthalmia, associated findings, and
97
the underlying diagnosis.
98
5
SMFM Fetal Anomalies Consult Series #1: Facial Anomalies smfm.org 99 100
Figure <02->1. Axial view of the fetal head and face showing the small and asymmetrical size of the orbits (calipers). This fetus has multiple other anomalies.
101
102 103 104 105 106 107 108 109
References 1. Busby A, Dolk H, Collin R, Jones RB, Winter R. Compiling a national register of babies born
110
with anophthalmia/microphthalmia in England 1988-94. Arch Dis Child Fetal Neonatal Ed 1998
111
Nov;79(3):F168-73.
6
SMFM Fetal Anomalies Consult Series #1: Facial Anomalies smfm.org 112
2. Mashiach R, Vardimon D, Kaplan B, Shalev J, Meizner I. Early sonographic detection of
113
recurrent fetal eye anomalies. Ultrasound Obstet Gynecol 2004 Nov;24(6):640-3.
114
3. Feldman N, Melcer Y, Levinsohn-Tavor O, Orenstein A, Svirsky R, Herman A, et al. Prenatal
115
ultrasound charts of orbital total axial length measurement (TAL): a valuable data for correct
116
fetal eye malformation assessment. Prenat Diagn 2015 Jun;35(6):558-63.
117
4. Abuhamad A, Charoui R. First Trimester Ultrasound Diagnosis of Fetal Abnormalities.
118
Philadelphia: Wolters Kluwer; 2018.
119
5. Benacerraf B. Ultrasound Diagnosis of Fetal Syndromes. Second ed. London: Churchill
120
Livingstone; 2008.
121
6. International Society for Prenatal Diagnosis, Society for Maternal Fetal Medicine, Perinatal
122
Quality Foundation. Joint Position Statement from the International Society for Prenatal
123
Diagnosis (ISPD), the Society for Maternal Fetal Medicine (SMFM), and the Perinatal Quality
124
Foundation (PQF) on the use of genome-wide sequencing for fetal diagnosis. Prenat Diagn 2018
125
Jan;38(1):6-9.
126
7
S0002-9378(19)31018-X
DOI:
https://doi.org/10.1016/j.ajog.2019.08.016
Reference:
YMOB 12838
To appear in:
American Journal of Obstetrics and Gynecology
Please cite this article as: Benacerraf BR, Bromley BS, Jelin AC, Anophthalmia and Microphthalmia, American Journal of Obstetrics and Gynecology (2019), doi: https://doi.org/10.1016/j.ajog.2019.08.016. This is a PDF file of an article that has undergone enhancements after acceptance, such as the addition of a cover page and metadata, and formatting for readability, but it is not yet the definitive version of record. This version will undergo additional copyediting, typesetting and review before it is published in its final form, but we are providing this version to give early visibility of the article. Please note that, during the production process, errors may be discovered which could affect the content, and all legal disclaimers that apply to the journal pertain. © 2019 Published by Elsevier Inc.
SMFM Fetal Anomalies Consult Series #1: Facial Anomalies smfm.org 1
Anophthalmia and Microphthalmia
2
Beryl R. Benacerraf, MD; Bryann S. Bromley, MD; Angie C. Jelin, MD
3 4
Introduction
5
Anophthalmia and microphthalmia are characterized by the complete or almost complete lack of
6
the primary optic vesicle, resulting in an absent or very small malformed orbital globe.
7 8
Definition
9
Anophthalmia is the complete absence of the orbital globe. Microphthalmia refers to a small
10
typically malformed orbital globe. These abnormalities can be unilateral or bilateral. The birth
11
prevalence of these two malformations combined is approximately 1 per 10,000 births (1).
12 13
Ultrasound Findings
14
The fetal orbits are typically detectable by 11–12 weeks’ gestation, and the lens is seen as a thin,
15
walled circle within each orbit by 13–14 weeks gestation (2). The diagnosis of anophthalmia or
16
microphthalmia is typically a subjective one, although orbital measurements at each gestational
17
age are available (3). The coronal view of the fetal face is the best way to evaluate the orbits.
18
This view can show the size and shape of the orbits, their positioning on the fetal face, spacing
19
between the two orbits, and associated facial abnormalities. The sagittal view of each orbit is
20
also helpful when measuring the size of the orbit. The lens is seen as a small, thin-walled,
21
circular structure and is normally visible in the anterior aspect of the globe in both the axial and
22
sagittal views. The hyaloid artery is visible traversing the middle of the eye from anterior to
23
posterior usually by 14 weeks and should disappear by 29 weeks (4). Most often, the detection of
1
SMFM Fetal Anomalies Consult Series #1: Facial Anomalies smfm.org 24
these rare but severe ocular anomalies is made because other fetal anomalies are present and the
25
orbital findings are part of a syndrome. Orbital defects are rarely discovered prenatally as
26
isolated findings(see Figure 1)
27 28
Associated Abnormalities
29
The associated anomalies vary with the fetal syndrome involved; therefore, it is crucial to
30
perform a thorough sonographic anatomic evaluation. Triploidy and trisomies 9 and 13 are
31
among the aneuploidies most likely to feature microphthalmia. Triploidy has early asymmetric
32
fetal growth restriction associated with anomalies of the heart, brain, and face (hypertelorism).
33
Trisomy 13 is associated with midline facial and brain defects as well as cardiac anomalies and
34
polydactyly. Trisomy 9 results in early pregnancy loss; survival generally only occurs in mosaic
35
cases. Features of mosaic trisomy 9 include abnormalities of the heart, face, and skull.
36
Nonsyndromic conditions that can feature microphthalmia include holoprosencephaly spectrum,
37
congenital viral infections (particularly rubella), and CHARGE association (Coloboma, Heart
38
defects, Atresia choanae (choanal atresia), growth Restriction, Genital anomalies, and Ear
39
anomalies). Other syndromes associated with eye anomalies include Aicardi syndrome (female
40
fetus, arachnoid cyst); Fraser syndrome (genitourinary and tracheal anomalies); Fryns syndrome
41
(congenital diaphragmatic hernia); Goldenhar syndrome (ear tags, cleft lip and/or palate,
42
asymmetry of face); Gorlin syndrome (ventriculomegaly); Lenz syndrome (microcephaly);
43
Walker-Warburg syndrome (lissencephaly, ventriculomegaly, cataracts); fetal alcohol syndrome;
44
and others (5).
45 46
Differential Diagnosis
2
SMFM Fetal Anomalies Consult Series #1: Facial Anomalies smfm.org 47
Anomalies of the fetal eye may be bilateral or unilateral and asymmetrical. Anophthalmia and
48
microphthalmia refer to the size of the globe and orbit. Congenital cataracts should not be
49
confused with microphthalmia, although both conditions may be present in the same fetus. The
50
orbit may be distorted by masses such as intracranial teratomas (associated with intracranial
51
component), gliomas (usually medial aspect of orbit), or retinoblastomas (rarely seen in utero).
52 53
Genetic Evaluation
54
Diagnostic testing (amniocentesis or chorionic villus sampling) with chromosomal microarray
55
analysis (CMA) should be offered when anophthalmia is detected. If screening or other
56
ultrasound features are suggestive of a common aneuploidy, it is reasonable to initially perform
57
karyotype or fluorescence in situ hybridization, with reflex to CMA if these test results are
58
normal. Many syndromes are associated with anophthalmia; they can be sporadic, autosomal
59
dominant, autosomal recessive, or X-linked. If there are additional anomalies, consanguinity, or
60
a family history of a specific condition, gene panel testing or exome sequencing may be useful,
61
as CMA does not detect single-gene (Mendelian) disorders. If exome sequencing is pursued,
62
appropriate pretest and posttest genetic counseling by a provider experienced in the complexities
63
of genomic sequencing is recommended (6). Maternal infections (rubella), vitamin A deficiency,
64
and teratogenic exposures (thalidomide) have also been associated with anophthalmia; therefore,
65
obtaining a history of maternal exposures and a family history is important. After appropriate
66
counseling, cell-free DNA screening is an option for patients who decline diagnostic evaluation
67
if a common aneuploidy is suspected.
68 69
3
SMFM Fetal Anomalies Consult Series #1: Facial Anomalies smfm.org 70
Pregnancy and Delivery Management
71
A detailed ultrasound examination should be performed and should include comprehensive
72
imaging of the intracranial structures (e.g., a neurosonogram) and the fetal heart. A fetal
73
echocardiogram, as well as fetal magnetic resonance imaging to assess for intracranial
74
abnormalities, should be considered. Referrals to pediatric ophthalmology, craniofacial clinic,
75
plastic surgery, or other subspecialty services should be based on additional sonographic
76
findings. Pregnancy termination is an option that should be discussed with all patients in whom a
77
fetal anomaly is detected. Shared patient decision-making requires a thorough evaluation and
78
multidisciplinary counseling regarding prognosis. The specific finding of anophthalmia or
79
microphthalmia does not generally affect delivery management, although delivery at a tertiary
80
care center with pediatric genetic, craniofacial, and ophthalmology consultation should be
81
considered, as appropriate for the clinical findings.
82 83
Prognosis
84
The prognosis is variable and dependent upon the severity, associated anomalies, and underlying
85
genetic etiology. Unilateral microphthalmia can have a favorable prognosis other than possible
86
blindness in the affected eye. Mild to moderate microphthalmia can be managed with
87
conformers, whereas severe cases may require surgical remodeling. Bilateral microphthalmia is
88
often associated with intellectual disability, and vision is dependent upon retinal development.
89
Reported cases of anophthalmia typically represent severe microphthalmia, as true, primary
90
anophthalmia is rarely compatible with life secondary to associated cerebral anomalies.
91 92
Summary
4
SMFM Fetal Anomalies Consult Series #1: Facial Anomalies smfm.org 93
Microphthalmia is a rare abnormality of the eye that generally occurs due to a genetic syndrome,
94
maternal infection, teratogenic exposure, or vitamin deficiency. Diagnostic testing is
95
recommended with CMA and/or molecular genetic testing based on associated anomalies.
96
Prognostic counseling is dependent on the severity of microphthalmia, associated findings, and
97
the underlying diagnosis.
98
5
SMFM Fetal Anomalies Consult Series #1: Facial Anomalies smfm.org 99 100
Figure <02->1. Axial view of the fetal head and face showing the small and asymmetrical size of the orbits (calipers). This fetus has multiple other anomalies.
101
102 103 104 105 106 107 108 109
References 1. Busby A, Dolk H, Collin R, Jones RB, Winter R. Compiling a national register of babies born
110
with anophthalmia/microphthalmia in England 1988-94. Arch Dis Child Fetal Neonatal Ed 1998
111
Nov;79(3):F168-73.
6
SMFM Fetal Anomalies Consult Series #1: Facial Anomalies smfm.org 112
2. Mashiach R, Vardimon D, Kaplan B, Shalev J, Meizner I. Early sonographic detection of
113
recurrent fetal eye anomalies. Ultrasound Obstet Gynecol 2004 Nov;24(6):640-3.
114
3. Feldman N, Melcer Y, Levinsohn-Tavor O, Orenstein A, Svirsky R, Herman A, et al. Prenatal
115
ultrasound charts of orbital total axial length measurement (TAL): a valuable data for correct
116
fetal eye malformation assessment. Prenat Diagn 2015 Jun;35(6):558-63.
117
4. Abuhamad A, Charoui R. First Trimester Ultrasound Diagnosis of Fetal Abnormalities.
118
Philadelphia: Wolters Kluwer; 2018.
119
5. Benacerraf B. Ultrasound Diagnosis of Fetal Syndromes. Second ed. London: Churchill
120
Livingstone; 2008.
121
6. International Society for Prenatal Diagnosis, Society for Maternal Fetal Medicine, Perinatal
122
Quality Foundation. Joint Position Statement from the International Society for Prenatal
123
Diagnosis (ISPD), the Society for Maternal Fetal Medicine (SMFM), and the Perinatal Quality
124
Foundation (PQF) on the use of genome-wide sequencing for fetal diagnosis. Prenat Diagn 2018
125
Jan;38(1):6-9.
126
7