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Next Article 
Blood, Vol. 91 No. 7 (April 1), 1998:
pp. 2213-2222
REVIEW ARTICLE
Hydrops Fetalis Caused by  -Thalassemia: An Emerging Health Care
Problem
By
David H.K. Chui and
John S. Waye
From the Provincial Hemoglobinopathy DNA Diagnostic Laboratory and
Department of Pathology, Faculty of Health Sciences, McMaster
University, Hamilton, Ontario, Canada.
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INTRODUCTION |
HYDROPS FETALIS is a serious disorder,
usually indicative of an ominous prognosis for the affected fetus.
There are many causes, including both hereditary and acquired
diseases.1-3 In southeast Asia,  -thalassemia is the most
common cause of fetal hydrops, accounting for 60% to 90% of the
cases.4-7 With population migrations during the past
decades, this syndrome is now seen in increasing numbers in other parts
of the world.
-Thalassemia is caused by mutations of the -globin genes, leading
to decreased or absent -globin chain production from the affected
genes. -Globin chains are the subunits for both fetal hemoglobin
(2 2) and adult hemoglobin
(2 2). Therefore, severe -thalassemias
can cause anemia in fetuses and in adults. Together with
-thalassemias which are caused by mutations of the -globin genes,
the thalassemias are among the most common single gene mutations in
humans.8 They are found mostly in areas where malaria was
and may still be endemic.
Each person normally has a total of four -globin genes, two of which
are encoded in tandem (in cis) on each chromosome 16 (Fig
1). There are -thalassemia deletions that remove
either one or two -globin genes on each chromosome
16.9-11,11a If both parents are carriers of a deletion
removing two -globin genes in cis on one chromosome 16, there is a
one in four risk that in each pregnancy, the fetus might inherit both
parental deletional mutations, and lack all -globin genes.
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| Fig 1.
Deletions in the -globin gene cluster. The -globin
gene cluster is located on the short arm of chromosome 16 near the
telomere. The three active globin genes,  2, 2, and 1, are
represented by red boxes, whereas the four pseudogenes are represented
by open boxes. The extent of the deletions are shown by the solid blue
lines. The (--HW) deletion encompasses more than 300 kb,
and is represented with arrows in the figure.26 The
 ()20.5 deletion spares the 2 gene, and removes the
2 gene and the 5 region of the 1 gene.29
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Because -globin chains normally are produced throughout gestation,
fetuses without -globin genes would suffer from severe anemia, and
thus hypoxia, heart failure, and hydrops fetalis. They would usually
survive in utero until the third trimester of gestation when they would
succumb to their genetic defects. In contrast to a normal fetus whose
major hemoglobin is Hb F (22), these
fetuses have primarily Hb Bart's (4). This disorder,
first described in 1960, is known as homozygous -thalassemia or Hb Bart's hydrops fetalis syndrome.12,13
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MOLECULAR AND POPULATION GENETICS |
The (--SEA) Deletion in Southeast Asia
The -globin gene cluster is made up of one embryonic -globin gene
(2), two -globin genes (2 and 1), and four pseudogenes. It
spans 30 kb and is located on the short arm of chromosome 16 near the
telomere (Fig 1). A major regulatory region, HS-40, is found 40 kb
upstream to the -globin gene and is indispensable for the expression
of -globin genes in cis.14,15
In southeast Asia, a common -thalassemia mutation is the
(--SEA) deletion. It is 20.5 kb in length, deleting both
-globin genes, but sparing the embryonic -globin gene (Fig
1).9-11 Homozygosity for this deletion,
(--SEA/--SEA), is the most common cause of the
Hb Bart's hydrops fetalis syndrome. The molecular basis of this
genetic disorder was deciphered in 1974, the first ever for human
diseases.16,17
The carrier rates of the (--SEA) deletion in southeast Asia
are high (Table 1), and there are considerable
variations in different regions.7,18-22 However, detailed
surveys are lacking. Among people of southeast Asian origin living in
the United States, 5.4% of them were found to be carriers of the
(--SEA) deletion, whereas 1% were found to be carriers of
the (--FIL) deletion (see the following
section).23,24
Large Deletions Which in Combination With (--SEA) Can
Cause Hydrops Fetalis
In southeast Asia, there are three known, large -thalassemia
deletions which remove all the - and -globin genes in cis, ie,
the (--FIL) deletion in the Philippines, the
(--THAI) deletion in Thailand, and the (--HW)
deletion measuring over 300 kb found in a Chinese family (Fig 1).25,26 Diagnostic strategies designed for the
(--SEA) deletion would not recognize these large deletions.
For Southern analysis, probes which are distal to the deletion
breakpoints, such as the LO, 3HVR (hypervariable region), and
5HVR, have to be used.24-26 Family studies often are
helpful.26 Recently, PCR methods with primers designed to
detect either the (--FIL) or the (--THAI)
deletions have been developed.26a,26b
In a survey of 1,500 people of Filipino ancestry living in Hawaii, the
carrier rate of the two -globin gene deletion is 10%, and
approximately 66% of these are of the (--FIL)
deletion.27 On the other hand, these large deletions are
uncommon in Hong Kong and Taiwan, accounting for less than 3% of those who are carriers of the two -globin gene deletion.7,18
It is generally accepted that fetuses homozygous for these large
deletions do not present with the Hb Bart's hydrops fetalis syndrome
because of their demise early in gestation (see the following section
on Pathophysiology).25 However, fetuses who are compound heterozygous for the (--SEA) deletion and one of these
large deletions, such as (--SEA/--FIL), develop
the Hb Bart's hydrops fetalis syndrome.25,26
Deletions Causing Hydrops Fetalis in the Mediterranean
Region
Hb Bart's hydrops fetalis has been reported in
Cyprus,28,29 Greece,30-33
Sardinia,34 and Turkey.35 It is caused by
either of two deletional mutations, (--MED) and
()20.5.29,32 These deletions are similar
to the (--SEA) deletion in that they remove or disrupt both
-globin genes, but not the -globin gene (Fig 1). Because they are
quite rare, Hb Bart's hydrops fetalis syndrome is not common in the
Mediterranean populations.36 In some cases, consanguinous
marriages are involved.34
Other -thalassemia Mutations
There are many other deletions which remove either two -globin genes
in cis, the entire --globin cluster which is sometimes designated
as (--Tot), or the HS-40 sequences, thus leading to the
silencing of the -globin gene expression.9-11,11a They
have been described in almost every population, and might contribute to
causing the hydrops fetalis syndrome. However, no such cases have been
recorded, mainly because these deletions are rare.
Deletions which remove only one single -globin gene on chomosome 16 are common.9-11 A person who is homozygous for these deletions would have a hematologic profile similar to one who is a
carrier of the (--SEA) deletion because functionally both
individuals possess two -globin genes. However, those who are either
heterozygous or homozygous carriers of the single -globin gene
deletions are not at risk for conceiving fetuses who will lack all
-globin genes. For example, even though single -globin gene
deletions are frequently found in people of African ancestry and in the
Indian subcontinent, Hb Bart's hydrops fetalis has not been reported
in these populations.37
Unusual -thalassemia Mutations Causing Hydrops Fetalis
There are rare reports in the literature describing fetuses with
the Hb Bart's hydrops fetalis syndrome who also had one
apparently normal -globin gene.7,38-41 Recently, the
genotypes of two such fetuses were described, one with
(--Tot/deletion of GAG in codon 30
) and the other one with
(--SEA/codon 59 GGC  GAC or GlyAsp
).41
A person with a single normal -globin gene, as a result of either
the deletion of three -globin genes, or a combination of two
-globin gene deletion and a point mutation of the third -globin
gene, ordinarily has the so-called Hb H disease. This person has
moderate anemia in adult life but usually without need for transfusion,
and no hydropic changes during fetal development.9-11 The
mechanisms and pathophysiology to account for the severe anemia and
hydropic changes of the two aforementioned fetuses remain to be
clarified.
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PATHOPHYSIOLOGY AND CLINICAL FINDINGS |
Hemoglobins in Normal and Hydropic Fetuses
During embryogenesis, there are three embryonic hemoglobins, Hb Gower 1 (2 2), Hb Gower 2 (22), and Hb Portland 1 (22). By 6 to 7 weeks postconception, the
production of embryonic - and -globin chains becomes almost
undetectable.42 Thereafter, the major hemoglobin in the
fetus is Hb F (22), and later
supplemented by less than 10% of Hb A
(22) until birth.43,44
In an embryo with a genotype of (--FIL/--FIL),
lacking the entire --globin gene clusters, the hemoglobins
present would be homotetrameric 4 and Hb Bart's
(4). These hemoglobins do not undergo heme-heme interaction and Bohr effect, and have very high oxygen
affinity.45 They are incapable of oxygen delivery to
tissues in the rapidly growing embryo. Therefore, it is generally
accepted that the affected embryo would succumb to severe hypoxia very
early in gestation, and miscarriage should ensue, thus precluding the
detection of these conceptions.25
Fetuses with a genotype of (--SEA/--SEA)
usually survive into the third trimester of gestation.9-11
This is generally attributed to the fact that the embryonic -globin
genes continue to be operative in these fetuses, leading to the
formation of about 10% to 20% embryonic Hb Portland 1 (22), and to a much lesser extent, Hb Portland 2 (22).46-49 Hb
Portland 1 possesses physiological oxygen dissociation capability and
can deliver oxygen to fetal tissues.50 Nevertheless, the
amounts of these hemoglobins are insufficient to keep pace with the
remarkable growth and development of the fetus, especially during the
third trimester of gestation. Ultimately the fetus would succumb to
hypoxia and heart failure either in utero or shortly after
birth.9-11
Fetal Abnormalities
The affected fetuses have decreased hemoglobin synthesis because of the
absence of -globin genes (Fig 2). Most
of the hemoglobin present is Hb Bart's (4) which is
unable to deliver oxygen to tissues, is relatively unstable, and can
precipitate and cause shortened red cell survival and possibly
ineffective erythropoiesis.45,51 These fetuses are usually
severely anemic, although in some, the hemoglobin level can be as high
as 100 g/L.10 The circulating erythrocytes are markedly
hypochromic and anisopoikilocytic (Fig 3).There are many nucleated erythroblasts in the peripheral blood, indicative of erythropoietic stress. Extensive extramedullary erythropoiesis is found in many organs and sites. This is the cause for
the massive hepatomegaly. The spleen can also be enlarged.
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| Fig 3.
Peripheral blood smear of the newborn shown in Fig 4.
Note the hypochromia, anisopoikilocytic changes, and
erythroblastosis.
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The change from - to -globin synthesis in a fetus normally is
completed by the sixth to seventh week postconception.42 Thereafter, in fetuses lacking -globin genes, severe anemia and fetal hypoxia would occur, which can adversely affect subsequent organogenesis and fetal development. One effect of anemia and hypoxia,
ie, placentomegaly, can be detected by ultrasonography in some fetuses
as early as the 10th week of gestation (see section on Prenatal
Diagnosis by Ultrasonography).52 In one series, 17% of
affected newborns were found to have congenital anomalies.5 They included hydrocephaly and microcephaly, as well as
cardiopulmonary, skeletal, and genitourinary malformations. In another
survey of 65 affected newborns in Thailand, severe reduction in brain
weight was noted in some.10 Hypoplasia of lung, thymus,
adrenals, and kidneys has been observed.53 Anomalous
genitalia were present in other infants.53-55 Recently,
limb reduction defects such as absence of hand and forefoot were
reported.55-57,57a
At birth, these newborns are usually pale, large and edematous,
sometimes with anasarca. However, not all affected newborns are grossly
hydropic (Fig 4A), illustrating the wide
spectrum of clinical presentations of this disorder. Often, there are
signs of high output heart failure, such as cardiomegaly, pericardial effusion (Fig 4B), pleural effusion, and ascites. The placenta is
massively enlarged.5
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| Fig 4.
Autopsy photographs of a newborn with hemoglobin Bart's
hydrops fetalis syndrome, delivered by caesarean section at 31 week of
gestation.59 Despite active resuscitation, the infant died within an hour after birth. Note edema of face and abdominal distension (A). The thoracic cavity is filled by the pericardial sac distended by
effusion and cardiomegaly; there is massive hepatomegaly (B). Pictures
courtesy of Prof H.A. Heggtveit.
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Maternal Complications
There is an increased incidence of serious maternal complications in
these pregnancies. It is likely that the placentomegaly is one
important causative factor. It was estimated that half of these women
could die from complications resulting from these pregnancies if there
was no medical care.10 In a study of 46 women who were
pregnant with affected fetuses, 61% developed hypertension during
pregnancy, of whom half developed severe pre-eclampsia.5 Polyhydramnios was present in 59% of the cases. Eleven percent suffered antepartum hemorrhage as a result of either unknown cause or
placenta previa. Other less common complications included disseminated intravascular coagulation, renal failure, and pleural effusion. Oligohydramnios, abruptio placenta, premature labor, and congestive heart failure have also been reported.53,54,58
The mean gestation at delivery was 31 weeks with a range of 24 to 38 weeks.5 Malpresentation of the infant during births occurred in 37% of the cases. Thirty-eight women delivered vaginally, 10 of whom experienced difficulty including 3 necessitating
paracenteses to decrease fetal ascites to facilitate delivery.
Caesarean section was performed in 8 women. Post-partum complications
include retained placenta, hemorrhage, life-threatening hypertension,
puerperal pyrexia, and anemia.6,54,59
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THE ONTARIO EXPERIENCE |
The Province of Ontario has a population of eleven million people.
There are 600,000 people of southeast Asian origins, such as China,
Hong Kong, Laos, the Philippines, Taiwan, and Vietnam. It is estimated
that annually in Ontario there are approximately 20 to 60 pregnancies
at risk for having fetuses with the Hb Bart's hydrops fetalis
syndrome.
From 1989 until 1997, the DNA Diagnostic Laboratory in Ontario has
performed prenatal tests for 50 pregnancies at risk of the
syndrome.60 Three of these pregnancies were at risk for both hydrops fetalis and Hb H disease. More than half (30/50) were
conducted on chorionic villus samples obtained during the first
trimester of pregnancy, while the remainder were on amniotic fluid or
amniocyte cultures obtained during the second trimester. Eleven fetuses
with homozygous 0-thalassemia were diagnosed, whereas 26 were carriers of 0-thalassemia, 2 were carriers of
+-thalassemia, and 11 were found to have the normal
complement of four -globin genes. These 50 pregnancies involved 37 couples. Only 4 couples at risk had been identified and counselled
before their first pregnancy. Fifteen couples were found to be at risk during their pregnancies. As many as half of the couples referred were
found to be at risk after they had one or more pregnancies ended with
hydropic newborns. These observations indicate the grossly inadequate
preconception carrier screening for -thalassemia in Ontario.
For the same period (1989-1997), there should have been several hundred
pregnancies at risk in Ontario. These figures indicate that despite the
availability of hospital-based genetic services, only 10% to 30% of
the at risk pregnancies in Ontario are identified and provided with
genetic counseling and diagnostic services. In the same period, the
Laboratory was called on to confirm 16 cases of hydrops fetalis caused
by -thalassemia. Three cases were diagnosed by ultrasound
examination, and later confirmed by DNA testing of fetal blood obtained
by cordocentesis. The remaining 13 cases were diagnosed by DNA testing
of cord blood at birth or fetal tissue obtained at autopsy.
The correct diagnosis of homozygous -thalassemia was sometimes
missed at autopsy of affected fetuses. In one case, the final autopsy
diagnosis was incorrectly ascribed to congenital heart disease. In
another case, the woman later became pregnant again and was found to
have an affected fetus again in the 24th week of the second pregnancy.
These observations suggest that the numbers of pregnancies with this
syndrome reported are likely to have been underestimated. Furthermore,
incorrect diagnosis can adversely affect the maternal health care
provided for subsequent pregnancies.
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TREATMENT AND PROGNOSIS OF SURVIVING INFANTS |
Counseling, Prevention, and Care for the Pregnant Woman
With very rare exceptions (see section below), all fetuses with the Hb
Bart's hydrops fetalis syndrome succumb to severe fetal hypoxia in
utero during the third trimester of gestation or within hours after
birth.9-11 The health care measures to combat this inevitably fatal disorder should be aimed at identifying couples at
risk in order to provide them with timely counseling, and prenatal diagnosis during early pregnancy. The screening tests to detect couples
at risk are simple blood counts and hemoglobin electrophoresis that are
widely available (see section on Carrier Detection and Prenatal
Diagnosis).
When such pregnancy is not diagnosed until the second trimester or
later, the emphasis should be to ensure the well-being of the pregnant
woman before and after delivery. When the diagnosis of an affected
fetus is confirmed, termination of the pregnancy should be possible
when requested by the pregnant woman, regardless of the stage of the
pregnancy.61
Postdelivery or Intrauterine Transfusions
There are now at least six surviving children born with homozygous
-thalassemia.55,62-67 These newborns either were
transfused immediately postdelivery or received intrauterine
transfusions. Their clinical courses are summarized in Table
2. All six children have been maintained on
a regular transfusion program, and iron chelation when appropriate,
similar to that for children with -thalassemia
major.68-70 Bone marrow transplantation is a possible future treatment modality for some. With proper medical therapy and
patients' compliance, significant progress has been made in the
survival of -thalassemia major patients, and similar prognosis is
anticipated for these six children with homozygous
-thalassemia.68-70 There are three other reports of
intrauterine transfusion to treat hydropic fetuses caused by
-thalassemia.41,71,74
These newborns often had serious neonatal complications. Some also had
congenital anomalies and delays in cognitive and motor functions. There
are ethical issues with regards to aggressive medical intervention in
fetuses who might harbor undiagnosed and possibly irreparable
developmental abnormalities caused by severe fetal hypoxia in utero
early during embryogenesis, and who would normally succumb to their
serious genetic defects.66 The high costs of such a
treatment program in light of the other societal needs and demands for
health care also deserve careful thought and discussion.66
In Utero Hemopoietic Stem Cell Transplantation
Intrauterine hemopoietic stem cell transplantation has been proposed as
another treatment alternative.72 Such a procedure was
performed in at least three pregnancies, all without
success.73-75 The ethical and societal issues raised in the
previous paragraph also apply to this form of medical intervention.
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CARRIER DETECTION AND PRENATAL DIAGNOSIS |
Screening for Couples at Risk
Ethnic origins.
This syndrome is found almost always in couples of southeast Asian
ancestry. Nevertheless, it has also been reported in the Mediterranean
populations.28-35 In practice, any person found to have low
erythrocyte mean corpuscular volume (MCV; see following section)
without iron deficiency should be considered a carrier of either -
or -thalassemia mutation.76-78 History of previous births of hydropic infants in a southeast Asian family should alert the
physician to the likely possibility of -thalassemia being present in
the family.
Low erythrocyte MCV.
The most important diagnostic criteria to detect thalassemia carriers
are microcytosis (MCV <80 fL) or hypochromia (mean corpuscular hemoglobin [MCH] <27 pg).9,77,78 In our laboratory,
the mean and SD of MCV and MCH for (--SEA/) carriers
are 67.8 ± 3.3 fL and 21.8 ± 1.2 pg, respectively. These laboratory
results should be routinely reported and included as part of the
prenatal screening records of all pregnant women.
On the other hand, adult carriers of two -globin gene deletion such
as (--SEA/) usually do not have significant
anemia.9 Our laboratory has found that the hemoglobin
levels for these men are 135 ± 10 g/L, and for women 121 ± 10 g/L.
Therefore, it behooves all physicians caring for people during their
adolescence or reproductive years to pay attention not only to the
hemoglobin values, but also to the MCV or MCH results. If one partner
of a couple is found to have microcytosis, the other partner should be
tested to determine if he/she also has microcytosis. If both have
microcytosis without iron deficiency, they should be investigated
further to determine if they are at risk for conceiving fetuses with
either Hb Bart's hydrops fetalis syndrome or -thalassemia
major.77,78
Hemoglobin electrophoresis.
Hemoglobin electrophoresis and Hb A2 levels are often
performed as part of the laboratory investigations to diagnose
thalassemia carriers. If the Hb A2 level is elevated
(>3.5%), the individual is considered to be a carrier of
-thalassemia mutation. If the Hb A2 level is normal or
low, the person is considered to be a carrier of -thalassemia
mutation.77,78 However, among people with microcytosis and
high Hb A2 levels, some are carriers of both - and
-thalassemia mutations.8,18,78a Of the 10 people diagnosed by our laboratory to be heterozygous carriers of both the (--SEA) -thalassemia deletion and a -thalassemia
mutation, their mean MCV is 72.3 fL (range, 66.9 to 78.4), and Hb
A2 level is 5.4% (range, 4.5 to 7.1). Therefore, the
-globin genotypes should be determined in all individuals who are
referred for investigation as possible thalassemia carriers.
Hb H inclusion bodies.
In adults carriers of -thalassemia mutations, there are excess
-globin chains within their erythroid cells. These -globin chains
can form homotetrameric Hb H (4) precipitates (inclusion bodies) on incubation with a redox agent such as brilliant cresyle blue
dye.79 The search for these inclusions is laborious and the
results are highly observer-dependent. Recent studies have suggested
that an immunocytological assay for embryonic -globin chains (see
below) or a polymerase chain reaction (PCR)-based DNA diagnostic
technique can serve as alternative screening
procedures.80,81
Embryonic -globin chains.
Adult carriers of the (--SEA) deletion have a very minute
amount of the embryonic -globin chains in their erythrocytes,
demonstrable by immunologic techniques with
anti-human-embryonic--globin-chain antibodies.82-87 In
particular, the immunocytological staining of peripheral blood smears
with the antibody has been shown to be highly sensitive and specific in
detecting adult carriers of the (--SEA)
deletion.60,84,87
Adult carriers of the large deletions such as the (--FIL)
deletion do not have detectable -globin chains in their
erythrocytes.87 If both partners are found to be negative
for the -globin assay, it is unlikely that they will conceive a
fetus with the Hb Bart's hydrops fetalis syndrome. Even if the embryo
did inherit both parental deletions, it should result in an early
miscarriage caused by the demise of the affected embryo.25
If both partners have microcytosis and only one is positive for the
-globin chain assay, both individuals then need to have definitive
DNA analysis to determine whether they are at risk of conceiving
fetuses with the Hb Bart's hydrops fetalis syndrome.87
Definitive Diagnosis by DNA Analysis for Couples at Risk
For genetic counseling and prenatal diagnosis, it is essential to
document the parental mutations at the DNA level either by Southern
blot analysis or by PCR-based strategies.60 There are
several PCR-based diagnostic protocols designed to identify the
(--SEA) and other -thalassemia
deletions.88-93 The diagnostic specificity of the PCR
techniques has to be rigorously maintained in view of recent reports of
misdiagnoses based on this strategy.94,95
Prenatal Diagnosis by DNA or Hemoglobin Analysis
Fetal tissue samples for DNA-based prenatal diagnosis are usually
obtained by chorionic villus biopsy (CVS) during 10 to 11 weeks of
pregnancy, or by aminocentesis during 16 to 20 weeks of pregnancy. The
risk for miscarriage in CVS is estimated to be 1.0%, and that for
amniocentesis to be 0.5%. Recently, a noninvasive method to obtain
fetal nucleated erythroblasts from maternal blood early in pregnancy
was reported.96,97 In all prenatal diagnoses, the
possibility of maternal tissue/blood contamination has to be guarded
against. In some instances, nonpaternity can also be a confounding
problem.
Fetal blood samples can be obtained by cordocentesis during the second
trimester of gestation. Both the DNA-based analysis and hemoglobin
electrophoresis can be performed on these blood samples. The major
hemoglobin found in a normal fetus during the second trimester of
gestation is Hb F (22), with 10% or less of Hb A (22). In a fetus with homozygous
-thalassemia, the major hemoglobin is Hb Barts (4),
with 10% to 20% of Hb Portland 1 (22),
and possibly some Hb H (4). Hb F or Hb A are not present in these fetuses. These results can be obtained rapidly by using simple
cellulose acetate electrophoresis. Similarly, cord blood samples
obtained at delivery and uncontaminated by maternal blood can be used
to genotype the newborn.
Prenatal Diagnosis by Ultrasonography
After the 20th week of gestation, ultrasound examination can readily
detect the many hydropic changes found in fetuses with the Hb Bart's
hydrops fetalis syndrome.54,98-101 A recent study reported
that hydropic changes in some fetuses could be detected as early as the
12th week of gestation.102
In a large study it was reported that increases in placental thickness
in some affected fetuses occurred as early as the 10th week of
gestation.52 By the 12th week, these measurements could identify most of the affected pregnancies. By the 18th week, the measurement could identify all affected pregnancies with a high specificity. These results were recently independently
confirmed.103
Fetal cardiothoracic ratio measurements were also useful to diagnose
affected fetuses.104 Taken together, ultrasound findings of
both placentomegaly and cardiomegaly at 12 to 14 weeks of gestation can
be highly specific for affected fetuses in pregnancies at risk.105 These measurements merit consideration as the next
best alternative to diagnose hydropic fetuses, particularly in places where Hb Bart's hydrops fetalis syndrome is common and where DNA-based prenatal diagnosis is not readily available.
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SUMMARY |
Recent advances in molecular genetics have provided insights into the
mutations and pathophysiology causing -thalassemias, as
well as definitive clinical diagnostic tests for adult carrier detection and prenatal diagnosis. Hydrops fetalis caused by
-thalassemia is found primarily though not exclusively among couples
of southeast Asian origin, and is encountered in increasing numbers in
North America and elsewhere.61,71,106-109,109a These
pregnancies inevitably result in fetal death during the third trimester
of gestation or shortly after birth, and frequently are associated with
serious maternal morbidity and even mortality.
Presently, most couples at risk for conceiving fetuses with this
serious genetic disorder are not identified. Other at risk couples are
recognized only after the birth of one or more hydropic newborns, or
hydrops fetalis is detected by ultrasonography during the second
trimester of a pregnancy. The correct diagnosis of these hydropic
fetuses is sometimes missed at autopsy. After experiencing the
horrendous obstetrical, medical, and psychosocial problems associated
with such pregnancies, many couples would decide against becoming
pregnant again, and some would even request
sterilization.61
A recurring theme of the many case reports of this syndrome is that the
correct diagnosis could have been made early in pregnancy, should the
physicians have been alert to this diagnostic
possibility.26,53,54,57-59,61-67,71,106-117 They reaffirm
the need for public education, both for the medical community and for
the population at large. Blood counts are often performed as part of
the medical examinations, particularly on all pregnant women during
their first visits to physicians. A low MCV result is the screening
test for carriers of the thalassemias.
With carrier detection, timely genetic counseling, and the availability
of prenatal diagnosis during early pregnancy, many couples at risk will
be spared of serious medical and psychological ordeals in their quest
for having families with children. It is therefore essential that this
genetic disorder is recognized, so that the appropriate maternal health
care and preventive measures can be provided to the affected couples
and communities.
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FOOTNOTES |
Submitted September 23, 1997;
accepted October 22, 1997.
Supported in part by the Medical Research Council of Canada, Cooley's
Anemia Foundation of New York, the US National Institutes of Health
(D.H.K.C.), the Ontario Thalassemia Foundation (J.S.W.), and the
Ontario Ministry of Health.
Address reprint requests to David H.K. Chui, MD, Department of
Pathology, Room 2N31, McMaster University Medical Centre, 1200 Main St
W, Hamilton, Ontario, Canada L8N 3Z5.
The publication costs of this article were defrayed in part by page charge payment. This article must therefore be hereby marked "advertisement" is accordance with 18 U.S.C. section 1734 solely to indicate this fact.
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ACKNOWLEDGMENT |
We wish to dedicate this review to the memory of the late Professor
W.H.C. Walker. His foresight, encouragement, and support were pivotal
in the establishment of the Provincial Hemoglobinopathy DNA Diagnostic
Laboratory. We are also indebted to our many clinical and laboratory
colleagues in Ontario and elsewhere for their advice and collaboration,
to Barry Eng, Margaret Patterson, and Shi-Ping Cai for their excellent
technical assistance, and to Lynne Lacey for her help in the
preparation of this manuscript.
| |
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< |
Introduction
References
Introduction