Primary ciliary dyskinesia: Kartagener syndrome in a family with a novel DNAH5 gene mutation and variable phenotypes


The Egyptian Journal of Medical Human Genetics (2015) 16, 95–99
H O S T E D  BY
Ain Shams University

The Egyptian Journal of Medical Human Genetics

www.ejmhg.eg.net
www.sciencedirect.com
CASE REPORT
Primary ciliary dyskinesia: Kartagener syndrome

in a family with a novel DNAH5 gene mutation
and variable phenotypes
Abbreviations: B–T shunt, Blalock–Taussig shunt; IVF, in vitro

fertilization; KS, Kartagener syndrome; KMGC, Kuwait Medical

Genetics Centre; PGD, preimplantation genetic diagnosis; S/P, syste-

mic-to-pulmonary.
* Corresponding author. Tel.: +965 24814328; fax: +965 24842073.

E-mail address: mj_marafie@yahoo.com (M.J. Marafie).

Peer review under responsibility of Ain Shams University.

http://dx.doi.org/10.1016/j.ejmhg.2014.08.001

1110-8630 � 2014 Production and hosting by Elsevier B.V. on behalf of Ain Shams University.
Makia J. Marafie *, Ibrahim S. Al Suliman, Abdullah M. Redha,

Abdulrahman M. Alshati
Kuwait Medical Genetics Centre, Maternity Hospital, Sabah Medical Area, P.O. Box 5833, Safat 13059, Kuwait
Received 6 June 2014; accepted 5 August 2014
Available online 22 December 2014
KEYWORDS

Arab;

Consanguinity;

DNAH5;

Kartagener syndrome;

Preimplantation genetic

diagnosis;

Primary ciliary dyskinesia
Abstract Background: Primary ciliary dyskinesia is a genetically heterogeneous autosomal

recessive disorder with variable clinical manifestations, including chronic rhinosinusitis, otitis

media, bronchitis, pneumonia, bronchiectasis, situs inversus totalis, reduced fertility in female

patients and male infertility. The condition occurs as a result of abnormal ciliary structure and func-

tion. It is presented in early life with an estimated incidence of approximately 1/16,000–20,000.

About 50% of the affected patients have situs inversus totalis leading to Kartagener syndrome

(MIM: 244400). So far more than 19 causative genes have been associated with primary ciliary

dyskinesia.

Case report: Here we are presenting Kartagener syndrome in a consanguineous Kuwaiti family

with a novel pathogenic DNAH5 gene mutation; namely c.9864dupA; [p.Pro3289ThrfsStop52],

which is predicted to result in protein truncation. In this family several homozygous individuals

showed variable disease manifestations.

Conclusion: Molecular test helped in confirmation of the clinical diagnosis and in providing bet-

ter management of the affected family members, which in turn could significantly improve overall

quality of their life. Consequently, preimplantation genetic diagnosis, which is the most acceptable

procedure in the Islamic countries, was offered to the heterozygous-carrier couple in order to pre-

vent recurrence of the disease in their future generations.
� 2014 Production and hosting by Elsevier B.V. on behalf of Ain Shams University.
1. Introduction

The name Kartagener syndrome (KS) came after the first
author who in 1933 described the triad of situs inversus, chronic
sinusitis and bronchiectasis as a distinct hereditary disorder [1].

KS (MIM: 244400) is a rare primary ciliary dyskinesia disease
(PCD). PCD is a genetically heterogeneous class of disorders

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96 M.J. Marafie et al.
known as ciliopathies, which are generally transmitted in an
autosomal recessive manner. However, other modes of inheri-
tance have been reported as well. These diseases have variable

clinical manifestations including chronic rhinosinusitis, otitis
media, bronchitis, pneumonia, bronchiectasis, situs inversus
totalis (mirror image orientation of thoraco-abdominal

organs), reduced fertility in female patients and male infertility.
PCD occurs as a result of abnormal ciliary structure and func-
tion affecting many tissues and organs. The disorganized ciliary

motions lead to impaired mucociliary clearance in the associ-
ated organs. These include the respiratory tract cilia, paranasal
sinuses, Eustachian tube, middle ear, oviduct, spermaductus,
flagella of sperm tail, brain and spinal cord ependyma [2]. Many

syndromes are linked to ciliopathies including, PCD/KS syn-
drome, Bardet–Biedl syndrome, hydrocephalus, polycystic kid-
ney disease, polycystic liver disease, nephrolithiasis, Meckel–

Gruber syndrome and Joubert syndrome. About 50% of the
affected patients have situs inversus totalis leading to KS.
PCD is presented in early life with an estimated incidence of

approximately 1/16,000–20,000 live births [3]. So far more than
19 causative genes have been associated with PCD: DNAH5,
DNAH11, DNAI1, DNAI2, RSPH9, RSPH4A, TXNDC3,

KTU/PF13, LRRC50, CCDC39, CCDC40, CCDC103,
HEATR2, LRRC6, DNAL1, DNAAF3, HYDIN, CCDC114,
CCDC164, CCDC65, c21orf59, SPAG1, ZMYND10, RSPH1,
ARMC4, and DYX1C1/DNAAF4. Moreover, RPGR, and

OFD1 are additional genes involved in syndromic forms of
PCD [4]. Mutations in DNAH5 gene located on chromosome
5p, is responsible for KS. DNAH5 encodes a protein associated

with the outer dynein arm of the cilia, and highly similar to the
Chlamydomonas c-dynein heavy chain [5,6]. Variable pheno-
types were observed with different mutations [6]. In this report

we discuss a Kuwaiti family with several cases of KS carrying a
novel homozygous DNAH5 gene mutation, and presenting dif-
ferent phenotypes.

1.1. Family data

The family presented here is a highly consanguineous Kuwaiti
family, in which double first cousin marriages have been fre-

quently practiced. In this family 5 cases of KS of variable
severity were observed.

1.2. Patient 1

This is the proband, a 27 year old female, who was referred by
the IVF unit at the Maternity hospital, for genetic counseling

and testing in preparation for preimplantation genetic diagno-
sis (PGD). She is the first cousin of her husband, had two chil-
dren with congenital heart disease (Fig. 1). The first child was a

boy, diagnosed antenatally with situs inversus totalis. He was
born at full term, after an uncomplicated pregnancy, with
complex cyanotic congenital heart disease. His medical report
revealed right atrial isomerism with dextrocardia, complete

atrioventricular septal defect with pulmonary atresia, supra-
cardiac total anomalous pulmonary venous connection (TAP-
VC) to left sided superior caval vein (right sided inferior caval

vein), and with S/P left sided BT shunt. He died postopera-
tively at the age of 6 weeks. Two years later she had her second
child (patient 2), a girl, born at full term with situs inversus
totalis (dextrocardia), but with no complication. She is cur-
rently 3 years old and doing well.

1.3. Patient 3

Proband’s mother was aged 56 years. Her parents were double
first cousins. She was also diagnosed with situs inversus totalis

with no complications throughout her life. She gave a history
of chronic sinusitis since childhood, requiring drainage and
myringotomy. Her mother had also situs inversus totalis, but

with a healthy life and no medical complications. However,
she died at the age of 57 years from stroke.

1.4. Patient 4

She was the first cousin of the proband, seen at the age of
19 years. Her parents were also consanguineous (Fig. 1). She
had no cardiac abnormalities. However, she gave a history

of recurrent middle ear infections and chronic sinusitis that
was treated several times with steroids. Her maxillary sinuses
were drained at the age of 12 years. She had myringotomy,

for three times, in both ears with pressure equalization tubes.
Her latest CT scan showed chronic inflammatory changes of
frontal and maxillary sinuses along with nasal septum devia-

tion, hypertrophic turbinates and nasal polyps. An endoscopic
sinus surgery with image guidance was planned for her. She
had two normal elder sisters and a younger brother. Addition-
ally, she had another brother who died at the age of 8 months

due to complex cyanotic congenital heart disease.
2. Methods

The written informed consent was obtained from the proband
and her adult relatives for blood collection and molecular test-
ing. The process involved 19 family members approaching

KMGC and requesting predictive gene testing. The genomic
DNA was extracted from the peripheral blood for defining the
carrier status of the involved subjects. Following PCR amplifi-

cation of the DNA, primary sequence analysis of the entire cod-
ing region of the commonly involved DNAH5 gene was
performed for the affected child (patient 2) and her grandmother

(patient 3). For other relatives targeted sequencing of both
familial mutation and alteration was performed separately, by
utilizing the following forward and reverse primers for each
exon respectively: Exon 58 Primers [F-50-TGCATTTT-

CAGCTGGATGTT-30, and R0-50GTCTGCCTCTTAAGCC
CTAA-30]; Exon 14 primers [F-50-GGGGCTGACATTGA-
TATGAT-30 and R-50-GAAGAGGGGTTCCCATGATT-30].

3. Result

Patients 2, 3 and 4 were found to be homozygous carrier for

the c.9864dupA; [p.Pro3289ThrfsStop52], in exon 58 of
DNH5 gene (Fig. 2). This is a pathogenic mutation predicted
to result in protein truncation, and describing the associated

clinical features. Additionally, all of them carried a homozy-
gous alteration in exon 14 of DNAH5 gene. This sequence var-
iant is defined as c.1853G>A, and predicted to result in the

amino acid substitution p.Arg618Gln. This sequence variant



Figure 1 Family pedigree. The proband (P1) is indicated by an arrow. The couple embarking on PGD is indicated by the star sign (*). P1:

patient 1, P2: patient 2, P3: patient 3, P4: patient 4.

Primary ciliary dyskinesia 97
is not predicted to abrogate known splice sites or disrupt splic-

ing. However, the mutation taster program (http://www.muta-
tiontaster.or) predicts the c.1853G>A; [p.Arg618Gln] to be a
disease causing variant.

Moreover, 9 other relatives were found heterozygous carri-

ers for the same pathogenic mutation in exon 58 as well as for
the sequence variant found in exon 14 of the same gene. These
were parents of patient 2 (patient 1 and her husband), grand-

father of patient 2, parents of patient 4, elder sister of patient 4
that was married to her first cousin, who was a carrier too, and
their two children (Fig. 1).
4. Discussion

KS is one of the PCD diseases that are inherited in an autoso-

mal recessive fashion. In Kuwait, similar to other Arab coun-
tries, the prevalence of consanguineous marriages is high and it
reached 54.3% [7]. Consequently, this leads to an increased

incidence of autosomal recessive disorders some of which are
rare and lethal [8,9]. In this report, pedigree analysis revealed
that the concerned family had practiced consanguinity over
many generations, and with many first cousin couples

(Fig. 1). Moreover, parents of patient 2 were first cousins,
her paternal grandparents were double first cousins, while
the maternal grandparents were second cousins. There is a his-

tory of other affected infants who died of similar heart condi-
tions, but we could not clarify this, as medical reports were no
longer available. Clinical manifestations varied between

affected individuals in this family; some had situs inversus
totalis with/or without respiratory tract disorders, one had
only respiratory tract problems and the closely related dead

boy had heterotaxy (lethal complex heart disease with right
atrial isomerism). In PCD, situs inversus was proposed to
occur as a random phenomenon due to loss of nodal ciliary
function, which is important for organ orientation during

embryogenesis [10]. Intra-familial phenotypic variability had
been observed in the literature [10,11]. Heterotaxy was
detected in 6.3% of individuals with PCD, and most of those
carried cardiovascular abnormalities. Moreover, it was fre-

quently associated with mutations in DNAI1 and DNAH5
genes [11]. However, no genotype phenotype correlation had
been detected in a cohort of patients selected from different

European and North American families, who were tested for
DNAH5 gene mutation in a study by Hornef et al. [12]. On
the contrary, screening of patients from Amish and Mennonite

communities revealed phenotypic variability in homozygous
carriers of the DNAH5 gene with 4348C>T founder mutation
[13]. Therefore, we are not sure whether the phenotypic vari-

ability in our family is associated with the mutation position
in the DNAH5 gene, or is simply due to the randomization
of left–right asymmetry. Hence genetic screening is a valuable
approach for assisting the diagnosis in patients with these

types of anomalies and should be applied in the clinical setting.
We have identified a disease-causing mutation in exon 58

of the DNAH5 gene; namely c.9864dupA; [p.Pro3289Thrfs-

Stop52] in a high-risk family. This pathogenic mutation is
novel and occurred in a homozygous state in the 3 available
affected individuals, and in a heterozygous state in 9 closely

related members of their family. Another variant was also
found in exon 14; c.1853G>A, in the same individuals; which
was in a homozygous state in the 3 affected members and in a
heterozygous state in the same 9 carriers of the pathogenic

exon 58; c.9864dupA mutation. Since we are not sure of the
pathogenicity of the latest, this will be screened for in the
embryos during the PGD processes. Molecular test helped

in confirmation of the clinical diagnosis in the affected
members, and in planning the future reproductive health
strategy for the heterozygous couples from this family. Patient

1 is currently under preparation for PGD using in vitro

http://www.mutationtaster.or
http://www.mutationtaster.or


Figure 2 Electropherogram of the homozygous mutation c.9864dupA (arrow), exon 58 of DNAH5 gene found in patient 2 and her

relatives. (A) Wild type. (B) Homozygous carrier. (C) Heterozygous carrier.

98 M.J. Marafie et al.
fertilization, in order to prevent recurring of the disorder in

the next pregnancy.

5. Conclusions

In the Arab communities the rate of autosomal recessive dis-
eases is high due frequently practiced consanguineous mar-
riages. A large number of these diseases are rare and
devastating. Therefore, efforts should be directed toward

planning intensive educational programs to increase the aware-
ness of the public about the possible outcome risks of
consanguineous marriages. Moreover, special emphasis should

be given to educate the health care professionals who are
involved in providing the premarital genetic services, in order
to recognize high-risk families with varieties of debilitating dis-

orders, to better manage these cases and to refer the selected



Primary ciliary dyskinesia 99
couples to the genetics clinics. Whereas clinical geneticists
should be trained for providing genetic counseling and screen-
ing, describing the reproduction options to couples at risk, and

for long term family health care management for the benefit of
their new generations. Finally, PGD procedure is the best pre-
vention option to avoid the birth of children with genetic dis-

orders in families who do not want to terminate the pregnancy
for any reason. However, it remains a financial problem for the
unfortunate low income families.

Note

There is no conflict of interest to the publication of this article.

Funding

No funding body was involved.

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	Primary ciliary dyskinesia: Kartagener syndrome  in a family with a novel DNAH5 gene mutation  and variable phenotypes
	1 Introduction
	1.1 Family data
	1.2 Patient 1
	1.3 Patient 3
	1.4 Patient 4

	2 Methods
	3 Result
	4 Discussion
	5 Conclusions
	Note
	Funding
	References