Sinan Sari

Prevalence of Celiac Disease in Healthy Turkish School Children

OBJECTIVES:Epidemiological studies of celiac disease (CD) in Turkey have been performed only within some regions of the country. The aim of this study was to determine the prevalence of CD in Turkish school children.METHODS:Between 2006 and 2008, serum samples were collected from 20,190 students (age range, 6–17 years) in 139 schools in 62 cities from different regions of Turkey. CD was screened using IgA antitissue transglutaminase (IgA-tTG) and total serum IgA. Subjects with selective IgA deficiency were further tested for IgG-tTG. Serum samples positive for IgA or IgG-tTG were further tested for IgA antiendomysial antibodies (IgA-EMAs) using an indirect immunofluorescence method. Small-intestinal biopsy was offered to all subjects with tTG antibody positivity.RESULTS:Of the 20,190 subjects, 489 were antibody positive (IgA-tTG only in 270, both IgA-tTG and IgA-EMA in 215, and IgG-tTG in 4). Selective IgA deficiency was detected in 108 patients, and 4 of them were positive for IgG-tTG. An intestinal biopsy was conducted in 215 subjects (IgA-tTG positive in 110, IgA-tTG and IgA-EMA positive in 104, and IgG-tTG positive in 1). The biopsy findings of 95 children were consistent with CD. Thus, the estimated biopsy-proven prevalence was 1:212 children. The positive predictive value (PPV) for IgA-tTG plus EMA was 75.9%. PPV was 44.3% when only IgA-tTG was used.CONCLUSIONS:We estimate that the prevalence of CD is at least 0.47% in healthy Turkish school children. Screening for IgA-tTG plus EMA provided better results for diagnosis when compared with testing for IgA-tTG alone.

Diversity of human rotavirus G9 among children in Turkey

Between September 2004 and December 2005 a prospective study was conducted to understand the epidemiology of rotavirus infection among children with diarrhea attending two hospitals in Ankara, Turkey. Rotavirus was detected in 39.7% of the 322 stool samples and affected mainly children in the age group of 6–23 months. More than 70% and 39% of these cases occurred in children <2 and <1 year of age, respectively. In the temperate climate of Ankara rotavirus infection was prevalent throughout the year. Serotype G1P[8] was dominant followed by G9P[8]. In 38 samples a total of 5 electropherotypes were detected. All G9P[8] were of long electropherotype except one of short electropherotype. A proportion of G1 and G9 strains were in combination with P[6], P[4] or P nontypable. Mixed serotypes were responsible for 2.4% of the infections. A phylogenetic tree constructed with the deduced amino acid sequences of the VP7 gene showed that 16 Turkish G9 strains clustered with rotaviruses of lineage III. One G9 strain formed a new lineage, lineage IV with the Sri Lankan G9 rotaviruses. In the phylogenetic tree of the VP8* gene, the Turkish G9P[6] rotaviruses clustered with human strains of lineage Ia. Increased diversity of the G/P type combination and the presence of infection throughout the year in Turkey was a situation similar to developing countries. The occurrence of rotavirus infection at later age and low level of mixed infections in Turkey represented the situation of developed countries. This study suggests that diverse G9 rotaviruses are emerging in Turkey. J. Med. Virol. 80:733–740, 2008.

Eponym: Papillon-Lefevre syndrome.

Papillon-Lefevre Syndrome (PLS) is a very rare autosomal recessive disorder characterized by palmoplantar hyperkeratosis and severe early onset periodontitis, affecting the primary and permanent dentition. The syndrome was first described by Papillon and Lefevre in 1924. Genetic, immunologic, and microbiologic factors are suggested as responsible for the initiation and progression of the disease. A point mutation of cathepsin C gene has recently been detected in PLS. A multidisciplinary approach is important for management .The prognosis has improved with the early recognition of the syndrome, effective professional supervision, and home care.

A variant Muckle-Wells syndrome with a novel mutation in CIAS1 gene responding to anakinra

Muckle-Wells syndrome (MWS) is a subset of autoinflammatory diseases. It is characterized by recurrent inflammatory crises associated with fever, abdominal pain, persistent urticaria, arthralgia, sensorineural deafness, and possible development of multiorgan amyloid A protein (AA)-type amyloidosis. Mutations in the CIAS1 gene have been reported in MWS. Interleukin 1B (IL-1B) probably plays a major role in the pathophysiology of the disease, and IL-1B blockade may be therapeutic for this syndrome. We report here a Turkish child with MWS treated with anakinra. A novel mutation (I480F) was identified in exon 3 of the CIAS1 gene in this patient. The resolution of inflammatory symptoms, normalization of serological values, and improvement in hearing was noted with anakinra treatment.

Primary Intestinal Lymphangiectasia in Children: Is Octreotide an Effective and Safe Option in the Treatment?

Objective: Octreotide has been suggested as a medical treatment option in refractory cases of primary intestinal lymphangiectasia (IL). There are few data about the long-term effect and safety of octreotide for IL in the literature. In the present article we analyzed pediatric cases of primary IL with long-term octreotide treatment and discussed its safety profile. Methods: Between 1999 and 2008, 13 children were diagnosed in our clinic as having IL. Six patients with primary IL were followed up, receiving octreotide therapy. The clinical data of the patients and duration of therapy, dose, and side effects of octreotide were evaluated. Results: Octreotide, 15 to 20 μg per body weight 2 times daily subcutaneously, was given to all of the patients. Duration of the octreotide treatment changed between 3 and 37 months. Stool frequency decreased in all of the patients after starting octreotide treatment. Serum albumin could be maintained at normal levels in 3 patients. The requirement of albumin infusions decreased in all of the patients. Acute pancreatitis was observed as a side effect of octreotide in 1 patient. Conclusions: Octreotide may help to maintain serum albumin levels, improve clinical findings, and decrease the requirement of albumin infusions in refractory cases of primary IL.

GRISCELLI SYNDROME: Description of a Case with Rab27A Mutation

A 7-month-old Turkish boy presented with partial albinism and typical clinical features of an accelerated phase, suggesting the diagnosis of Griscelli syndrome. The diagnosis was confirmed by light microscopic evaluation of hair and a peripheral blood smear. Genetic analysis identified a mutation in the Rab27A gene. He was initiated immunosuppressive treatment but accelerated phase could not be ameliorated. He unfortunately died from multiorgan failure. The finding of partial albinism in children should alert clinicians to consider Griscelli syndrome since simple methods can corfirm the diagnosis and early diagnosis is life-saving.

A Successful HSCT in a Girl with Novel LRBA Mutation with Refractory Celiac Disease

To the Editor The gastrointestinal tract is the largest lymphoid organ in the body. One of the major functions of the gastrointestinal tract is maintaining of the balance between active immunity, tolerance and immunosuppression. Dysregulation of this physiologic process can lead to diseases such as food allergy, celiac disease (CD) or inflammatory bowel disease [1]. Therefore, gastrointestinal symptoms such as chronic diarrhea and malabsorption might be indicative of primary immunodeficiency diseases [1]. A 10-year-old girl referred to our clinic with a six-year history of chronic watery diarrhea and unresponsiveness to a gluten free diet. She had been evaluated and treated previously for chronic diarrhea, intermittent fever, recurrent pneumonia, candida esophagitis, pancytopenia, hypoalbuminemia, hypolipidemia, vitamin B12 and folic acid deficiencies. She was diagnosed with CD, based on serologic and histopathological findings. She was placed on a strict gluten free diet for a year, but diarrhea did not improve. She has two healthy brothers. Her parents were consanguineous. On physical examination, she was cachectic; with height for age below 3 % (height SDS −5.18) and weight for age below 3 % (weight SDS −5.27). Bone age and height age of the patient were 6 years, 10 months and 5 years, 3 months, respectively. She had protuberant abdomen and clubbing. Liver and spleenwere palpable at 1 cm and 4 cm below the costal margins. Laboratory tests revealed mildly increased liver transaminases. Hemoglobin was 8.32 g/dl; MCV, 85 fL; RDW, 23.4 %; white blood cell, 5570/mm; platelet, 230,000/mm; reticulocyte count, 1 % and ferritin, 2.8 ng/ml. Coombs test was negative. Sedimentation rate was 18 mm/h, C-reactive protein, 1.78 mg/dl. Stool examinations were normal. 25-hydroxi vitamin D level was 25.7 ng/ml. Insulin like growth factor 1 (IGF-1) was 3.5 ng/mL (Normal, 108–648 ng/mL) and insulin like growth factor binding protein (IGFBP-3), 580 ng/mL (Normal, 2690–7200 ng/mL). Stimulated IGF-1 and IGFBP-3 were 2.85 ng/mL and 720 ng/mL, respectively, both markedly reduced. Basal and stimulated growth hormone levels were compatible with growth hormone insensitivity (12.9 ng/mL and 9.79 ng/mL, respectively). Anti-tissue transglutaminase IgA was positive with a titer of 200 IU/ml. Thyroid auto-antibodies, anti-saccharomyces cerevicea antibody and pANCA were negative. Bone mineral density showed severe osteoporosis (Z score, −5). Chest X-ray showed reticular density in the parenchyma of the lung. High-resolution chest tomography showed bilateral tubular bronchiectasis. Smear staining for acid resistant bacteria and tuberculosis PCR, and culture were negative. Upper gastrointestinal endoscopic examination revealed scalloping in the duodenal mucosa. Colonoscopy showed nonspecific Buket Dalgic and Aydan Ikinciogullari contributed equally to this work.

CD55 Deficiency, Early-Onset Protein-Losing Enteropathy, and Thrombosis

Background Studies of monogenic gastrointestinal diseases have revealed molecular pathways critical to gut homeostasis and enabled the development of targeted therapies. Methods We studied 11 patients with abdominal pain and diarrhea caused by early‐onset protein‐losing enteropathy with primary intestinal lymphangiectasia, edema due to hypoproteinemia, malabsorption, and less frequently, bowel inflammation, recurrent infections, and angiopathic thromboembolic disease; the disorder followed an autosomal recessive pattern of inheritance. Whole‐exome sequencing was performed to identify gene variants. We evaluated the function of CD55 in patients’ cells, which we confirmed by means of exogenous induction of expression of CD55. Results We identified homozygous loss‐of‐function mutations in the gene encoding CD55 (decay‐accelerating factor), which lead to loss of protein expression. Patients’ T lymphocytes showed increased complement activation causing surface deposition of complement and the generation of soluble C5a. Costimulatory function and cytokine modulation by CD55 were defective. Genetic reconstitution of CD55 or treatment with a complement‐inhibitory therapeutic antibody reversed abnormal complement activation. Conclusions CD55 deficiency with hyperactivation of complement, angiopathic thrombosis, and protein‐losing enteropathy (the CHAPLE syndrome) is caused by abnormal complement activation due to biallelic loss‐of‐function mutations in CD55. (Funded by the National Institute of Allergy and Infectious Diseases and others.)

ACOX2 deficiency: A disorder of bile acid synthesis with transaminase elevation, liver fibrosis, ataxia, and cognitive impairment

Significance Liver disease of unknown cause represents an unmet medical need. Using exome sequencing, we describe a syndrome associated with homozygous loss of Acyl CoA Oxidase 2 (ACOX2) featuring elevated transaminase levels, liver fibrosis, ataxia, and cognitive impairment. ACOX2 encodes the peroxisomal branched-chain acyl-CoA oxidase and is involved in the bile acid biosynthetic pathway. Importantly, this disorder is potentially reversible, because the bile acid synthetic pathway can be suppressed with exogenous bile acids, diminishing the production of the toxic metabolites likely causing liver and neurologic dysfunction. This study provides the means to diagnose ACOX2 deficiency in patients with chronic idiopathic liver disease and/or cryptogenic cirrhosis. Acyl CoA Oxidase 2 (ACOX2) encodes branched-chain acyl-CoA oxidase, a peroxisomal enzyme believed to be involved in the metabolism of branched-chain fatty acids and bile acid intermediates. Deficiency of this enzyme has not been described previously. We report an 8-y-old male with intermittently elevated transaminase levels, liver fibrosis, mild ataxia, and cognitive impairment. Exome sequencing revealed a previously unidentified homozygous premature termination mutation (p.Y69*) in ACOX2. Immunohistochemistry confirmed the absence of ACOX2 expression in the patient’s liver, and biochemical analysis showed marked elevation of intermediate bile acids upstream of ACOX2. These findings define a potentially treatable inborn error of bile acid biosynthesis caused by ACOX2 deficiency.

Nasal septal perforation in an adolescent girl with Crohn's disease: a rare extraintestinal manifestation.

Crohns Disease (CD) is a chronic granulomatous inflammatory bowel disease which may also involve the extraintestinal organs such as joints, liver, skin and perianal tissue. Involvement of the aerodigestive tract is quite rare in CD. We report a 16-year-old girl with CD and nasal perforation as an extraintestinal manifestation of the disease.