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Central European Journal of Immunology
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2/2013
vol. 38
 
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Review paper
The 22q11 microdeletion syndrome in children

Aleksandra Lewandowicz-Uszyńska
,
Katarzyna Zwonarz
,
Joanna Chmielarska

(Centr Eur J Immunol 2013; 38 (2): 271-275)
Online publish date: 2013/07/08
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Introduction

DiGeorge syndrome (often referred to as the 22q11.2 deletion syndrome) is one of well-defined primary immunodeficiency disorders associated with large defects [1]. The syndrome was described for the first time in 1968 by Angelo DiGeorge [2]. The literature still describes a similar coexistence of deficiencies, operating under the names:

• thymic hypoplasia with concomitant hypocalcemia,

• Takao syndrome (conotruncal anomaly face syndrome),

• velo-cardio-facial syndrome (VCFS, Shprintzen syndrome),

• Cayler cardiofacial syndrome,

• Opitz syndrome: genitourinary system irregularities in addition to cleft palate, heart defects and mental retardation,

• CATCH-22 syndrome (an acronym formed from the first letters of observed disorders: C – cardiac defects, A – abnormal faces, T – thymic hypoplasia, H – hypocalcemia from parathyroid aplasia, 22 – chromosome 22 microdeletions).

The syndrome affects 1 in 3000-5000 live births. 90% of cases are 22q11.pter chromosome deletions (mostly microdeletions) or 10p13 deletions (much less often) [3]. It is assumed that 72-90% of cases are a de novo genetic defect. The remaining patients have an autosomal dominant mutation inherited from the father or mother (three times more), and therefore discrete features of dysmorphia are observed in parents (they are asymptomatic carriers of the 22q11.2 microdeletion) [4, 5]. The risk of the syndrome in any subsequent child is 1 : 2 (50%).

The defect can be detected by fluorescence in situ hybridization (FISH) that uses probes targeted only to a critical region [3, 6-8]. MLPA. Due to the high variability of symptoms with the same kind of a genetic defect (loss of genes in the 22q11.2 region), the medical image probably also depends on a group of other genes, and therefore it cannot be prenatally determined based on diagnosed microdeletions whose symptoms will occur. Therefore, due to a large variability of the clinical picture, it is currently recommended to use the term “22q11.2 microdeletion syndrome”. The presence of characteristic mutations detected using the FISH technique is not confirmed in approximately 10% of patients diagnosed with the symptoms of the 22q11.2 microdeletion syndrome, because 10p13, 17p13 and 18q21.30 deletions or defects within individual genes are also possible.

The symptoms of the syndrome relate to different systems and organs in the form of disorders (they can occur in a variety of interrelations):

• absence or dysfunction of the thymus and the associated immune disorders,

• facial defects and abnormalities,

• cardiovascular abnormalities,

• metabolic and endocrine disorders,

• urological and nephrological abnormalities,

• neurological disorders.

In view of the wide variety of clinical pictures, criteria of definitive, probable and possible diagnosis have been developed to facilitate the diagnosis (Table 1) [8, 9].

Immune disorders

T lymphocytes are divided into subpopulations having different functions and characterized by a specific pattern of surface antigens. Differentiation of T cells occurs in the thymus. Precursors of T lymphocytes from bone marrow penetrate the cortical part of the thymus through the circulatory path and differentiate into thymocytes (CD4+, CD8). There is a positive selection of T cells in the cortex, but this refers only to cells that recognize MHC antigens through their TCR receptors. The others undergo apoptosis. Subsequently, the cells migrate into the cortical part of the thymus where in the course of further maturation, with the use of chemokines, the expression of surface antigens and antigen receptors specific to T cells occurs. A negative selection in turn takes place in the cortical part whereby cells highly reactive to self-antigens are eliminated. The process of the negative selection results in a loss of approximately 90% of the thymocyte population. At this stage, thymocytes eventually differentiate into cells that have only one of the antigens, CD4 or CD8, and are exported to the periphery [10].

Very frequently no thymus shadow on chest X-ray films is found in patients with the 22q11.2 microdeletion syndrome, which is of diagnostic importance and involves the presence of abnormalities in cellular and/or humoral immunity (deficit of T cells, especially CD4+, deficiency of major classes of immunoglobulins, IgG subclasses and specific antibodies) (Table 2). There are two forms of this syndrome: complete with severe impairments of cellular response and impaired humoral response, and partial in which the immune response is slightly impaired, and spontaneous remission of these irregularities is possible. A PHA-stimulated lymphocyte proliferation assay is useful in determining the form of the syndrome [11]. The response to vaccination is most often correct in the majority of patients diagnosed with impaired synthesis of specific antibodies (in patients with incomplete 22q11.2 microdeletion syndrome) [12]. An increased incidence of adverse vaccine reactions is not observed in this group [13]. Immunization with live vaccines is contraindicated in the case of low T-cell values or it should be postponed until the anomalies are resolved.

Data available in the literature show that 80% of immune abnormalities observed in the neonatal period may subside spontaneously in the first years of life [14]. It is now believed that in children with congenital absence of thymus or thymus removed during a cardiac surgery, the maturation and differentiation of T lymphocytes still occur outside the thymus, presumably from T lymphocytes present in the gastrointestinal tract [15]. The immune system disorders result in recurrent infections of the respiratory and gastrointestinal tracts, most often of viral, fungal and protozoan aetiology and less often of bacterial etiology.

The occurrence of immunodeficiency in the 22q11.2 microdeletion syndrome is also related to an increased risk of autoimmune disease, as in other types of PID [16]. Juvenile idiopathic arthritis, Graves-Basedow disease are observed [17, 18]. Thrombocytopenia and haemolytic anaemia are also observed but the frequency is not known. The cytopenias and other autoimmune diseases are more prone due to altered T regulatory homeostasis [19].

Facial defects and abnormalities

Dysmorphic facial features are also characteristic of the syndrome. They include an anti-mongoloid position of the eyelids, widely spaced eyes, and the so-called fish mouth caused by an underdeveloped lower jaw and short philtrum, and small low-set ears.

Other abnormalities often relate to the palate and may be the first symptoms of this syndrome. They can be manifested by feeding difficulties – frequent regurgitation of food, swallowing disorders. For this reason, children can inadequately put on weight. These problems may be caused by velopharyngeal insufficiency (the largest number of cases) resulting from muscular hypotonia which can be directly accompanied by the submucosal cleft palate, open cleft palate, cleft lip or tongue, which will greatly enhance the observed abnormalities [20].

Cardiovascular abnormalities

Defects in the circulatory system are the most important problem of patients with the 22q11.2 microdeletion syndrome. The severity of the defect and the possibility of cardiac surgery directly affect the survival of children with this syndrome [21]. The most common abnormalities include a syndrome of defects known as tetralogy or pentalogy of Fallot, common truncus arteriosus, transposition of the great arteries. Other less common defects include narrowing of the aortic orifice, pulmonary valve stenosis, right aortic arch and syndromes which combine the specific defects. A heart defect may not occur in about 26% of cases, and these are the most common cases of unrecognized 22q11.2 microdeletion syndrome. As a result of an increased availability of cardiac surgery centres and improved surgical techniques, children with the most severe cardiovascular defects survive and require further multidisciplinary care.

Metabolic and endocrine disorders

Metabolic and endocrine disorders occur especially in the form of hypocalcemia due to underdevelopment of the parathyroid glands, which results in low levels of PTH (parathyroid hormone). In extreme cases, these disorders can cause tetany [22], or errors – diagnosis of epileptic seizures. They are treated with calcium and vitamin D. The symptoms are most common in the neonatal period, with a tendency to disappear around 12-14 months of age. Symptoms of tetany, as a sign of increased demand for calcium, may also occur in older children, especially in adolescence, or in situations of stress, surgery, or in pregnant adults.

Urological and renal abnormalities

Abnormalities of the urinary tract may also occur in the course of the syndrome [23]. Devriend et al. [24] report on 4 renal and urological malformations among 37 cases of DiGeorge syndrome confirmed by genetic testing. Palacios et al. [25] report on pathology within the kidneys and ureters in as many as 7 of 11 patients with this syndrome.

Anomalies in the construction of kidneys and the urogenital tract (hypospadias) may cause nocturnal enuresis, abnormal urination, or recurrent urinary tract infections, which requires constant care or urological and renal correction [26].

Neurological and psychiatric disorders

Epilepsy or vertigo sometimes occurs in the syndrome. At a later age concentration, learning, and abstract thinking difficulties may take place [27]. There may also be adaptive disorders in the peer group due to pronunciation difficulties resulting from impaired speech organs. Serious mental disorders such as schizophrenia, depression or bipolar disorder are more often found in the population than in healthy people [28]. The reasons are seen not only in the chromosomal abnormalities, but also in chronic stress and anxiety as a result of childhood experiences (surgery, exposure to pain) [29].

Therapy in DiGeorge syndrome

Treatment of patients with DiGeorge syndrome has to be comprehensive and multidisciplinary. There is a need for life-saving cardiac surgery (heart defect), and surgery (cleft palate, cleft lip), genetic counselling and genetic testing. In some patients with the deep T lymphocyte deficit with concomitant severe infections and, in some patients with a decrease in the immunoglobulins level, the use of immunoglobulins either as a regular substitution or as an adjuvant therapy in the course of infection, depending on the clinical situation, is recommended. Immunization with live vaccines is contraindicated in patients with a severe immune deficiency (especially in terms of the number and function of lymphocytes). Vaccinations can be implemented in the incomplete 22q11.2 microdeletion syndrome as no increased incidence of adverse vaccine reactions is observed.

Microdeletion syndrome patients after cardiac surgery still require multidisciplinary care. As in other primary immunodeficiencies, there is an increased risk of developing tumours of the immune system cells in this syndrome. These patients require the so-called oncological vigilance and observation in the direction of autoimmune diseases, but these diseases are less common. Children with this syndrome also require care in the field of the so-called early intervention such as occupational therapy, rehabilitation (physical and of speech disorders), educational and psychological support.

The hematopoietic stem cells transplantation was suggested in cases of DiGeorge syndrome but severe symptoms of autoimmunity are the clinical indication. In these cases, the stem cell transplantation is successful, which supports the hypothesis that not the number of T lymphocytes but the defect of the T cell function is responsible for clinical symptoms in DiGeorge syndrome [5].



The authors declare no conflict of interest.

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Copyright: © 2013 Polish Society of Experimental and Clinical Immunology This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial-ShareAlike 4.0 International (CC BY-NC-SA 4.0) License (http://creativecommons.org/licenses/by-nc-sa/4.0/), allowing third parties to copy and redistribute the material in any medium or format and to remix, transform, and build upon the material, provided the original work is properly cited and states its license.
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