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Central European Journal of Immunology
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Case report

Diagnosis of autoimmune neutropenia in a 10-month-old boy – a case report

Katarzyna Zdanowicz
1
,
Urszula Daniluk
1
,
Elena Jewsiejenko
1
,
Milena Krasnodębska
1
,
Radosław Motkowski
2
,
Dariusz Marek Lebensztejn
1

  1. Department of Pediatrics, Gastroenterology, Hepatology, Nutrition and Allergology, Medical University of Bialystok, Poland
  2. Department of Pediatrics, Rheumatology, Immunology and Metabolic Bone Diseases, Medical University of Bialystok, Poland
Cent Eur J Immunol 2021; 46 (1): 118-120
Online publish date: 2021/03/11
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Introduction

Neutrophils play an important role as part of the innate immune system, and their reduced number may be associated with an impaired immune response. The term neutropenia is used to define a reduction in absolute neutrophil count (ANC) below 1500/µl, which may increase the risk of life-threatening infections, especially in the case of agranulocytosis (ANC < 100/µl) [1]. Neutropenia, congenital or acquired, is associated with impaired production of granulocytes in the bone marrow or increased peripheral destruction. Autoimmune neutropenia is caused by destruction due to autoantibodies directed against various neutrophil-specific antigens (HNA) [2].

We present a 10-month-old boy admitted to our department because of severe irritability with skin abscess formation and neutropenia.

Case report

A 10-month-old male infant with strong anxiety observed for one day was admitted to our department. Past medical history revealed surgery at the age of 8 months due to a Morgagni-Larrey hernia. In addition, the child was under the care of a cardiology outpatient clinic (ventricular septal defect type 2) and ENT outpatient clinic (bilateral sensorineural hearing loss). There were no abnormalities in complete blood counts and routine biochemical laboratory tests performed two and four months prior to hospitalization. The family history was insignificant. Physical examination revealed pale skin, postoperative scars, Mongolian spot in the sacral region, flat forehead, broad nasal bridge with a tendency to form epicanthal folds, single transverse palmar creases, persistent fetal pads, aphthous stomatitis, umbilical hernia and systolic murmur along the left border of the sternum. Preliminary results of laboratory tests showed agranulocytosis, monocytosis, anemia, and increase in C-reactive protein concentration. The results of laboratory tests are presented in Table 1. There were no abnormalities of abdominal organs based on abdominal radiographs and ultrasound examination, except for umbilical hernia.

Table 1

Results of laboratory tests

ParameterLaboratory resultsNormal range
4 months before admissionday of admissiondischarge
White blood cells [K/µl]10.676.575.195.0-12
Neutrophils [K/µl]2.70.1310.1551.5-7
Monocytes [K/µl]0.841.9051.0890.3-0.82
Hematocrit [%]32.824.535.534-40
Mean corpuscular volume [fl]72.575.175.975.00-86.00
Hemoglobin [g/dl]10.88.012.211.0-14.0
Platelet [K/µl]394685350140-450
C-reactive protein [mg/l]13.564.270-5
Creatinine [mg/dl]0.260.17-0.42
Alanine transferase [U/l]120-29
Procalcitonin [ng/ml]0.06< 0.5
Triglycerides [mg/dl]11035-150
Total cholesterol [mg/dl]120120-200
Immunoglobulin G [g/l]11.003.50-11.80
Immunoglobulin M [g/l]0.840.36-1.04
Immunoglobulin A [g/l]0.780.36-1.65
Glucose [mg/dl]7660-100
Lipase [U/l]1613-60
Ammonia [µmol/l]36.321-50
Lactate [mmol/l]1.590.50-2.20
Uric acid [mg/dl]4.61.1-5.5
Complement C3 [mg/dl]166.0090-180
Complement C4 [mg/dl]19.0010-40
Anti-CMV IgMnegativenegative
Anti-EBV IgM, IgGnegativenegative
HNA-1 antibodiespositivenegative
Fecal elastase-1 [µg/g]473.3> 200

On the second day of hospitalization, the tender and painful mass about 2 × 2.5 cm, without splashing in the right submandibular area was palpated. Ultrasound examination of this area revealed the features of a forming abscess. An laryngological consultation was performed and initially empiric antibiotic therapy with amoxicillin and clavulanic acid was used, but without improvement. On the seventh day of hospitalization under general anesthesia, a surgical incision and drainage of the abscess were performed. The pus culture indicated methicillin-sensitive Staphylococcus aureus (MSSA) infection. Due to agranulocytosis, immunological, genetic and hematological consultations were carried out to plan diagnostic tests to determine the cause of neutropenia. Epstein-Barr virus and cytomegalovirus infections were excluded. The lipid profile (total cholesterol and triglycerides), lactate and uric acid were within normal limits. The concentrations of elastase I and fat in the stool were normal; therefore exocrine pancreatic insufficiency was excluded. Urine organic acid analysis by gas chromatography-mass spectrometry (GC-MS) did not indicate inborn errors of metabolism. Immunophenotyping by flow cytometry was also performed and reference ranges for peripheral blood lymphocyte subsets were revealed. The immunoglobulin classes A, G, M, complement component 3 and complement 4 were within the normal range. Finally, anti-human neutrophil antigen-1 (HNA-1) antibodies were detected in serum using the granulocyte immunofluorescence test (GIFT), confirming an autoimmune neutropenia. Bone marrow biopsy was not performed due to parental disagreement. During hospitalization, the parents also refused to undergo genetic tests. After obtaining the culture result, antibiotic therapy was applied according to the antibiotic susceptibility testing. On the 14th day of hospitalization, the boy was discharged in good general condition with the recommendation of antibiotic prophylaxis (amoxicillin 20 mg/kg/24 h) until the follow-up visit at the immunological clinic. Our patient did not develop infectious diseases after starting prophylaxis with amoxicillin during 6 months of follow-up despite ANC < 500/µl.

Discussion

The causes of neutropenia are congenital disorders such as Shwachman-Diamond syndrome (SDS), Kostmann syndrome (KS), cyclic neutropenia (CyN), glycogen storage disease type 1b (GSD1b), primary immunodeficiency (PID) and organic acidemias. Acquired neutropenia may be induced by drugs, infections, leukemia, and autoimmune diseases. An example is autoimmune neutropenia of infancy (AIN), which was diagnosed in our patient [2].

The prevalence of AIN in children is 1 : 100,000, making it one of the most common causes of neutropenia in the pediatric population [2]. However, current research may suggest that previous data were underestimated based on the report of Farruggia et al. determining the incidence of AIN as 1 : 6,300 in children in Italy. AIN is diagnosed mainly at the age of 5-15 months and is more often observed in premature babies, which may be due to the immaturity of the immune system [3]. In most cases, the clinical course of AIN is mild. The most common manifestations of AIN in infants are upper respiratory tract infections, otitis media, pyoderma, fever of unknown origin, and gastroenteritis. More serious complications caused by Gram-positive and Gram-negative bacteria and fungal infections, such as pneumonia, sepsis or meningitis, are less common [4]. Our patient had a skin abscess due to a Gram-positive bacterial infection. The hematological abnormalities observed in AIN include isolated neutropenia or neutropenia in combination with anemia and/or thrombocytopenia and/or peripheral monocytosis; however, bone marrow examinations may show normal or increased cellularity with normal or low numbers of mature neutrophils. Detection of anti-neutrophil antibodies is a major step in confirming the diagnosis of AIN, although their detection is difficult due to low titer and avidity [5]. The presence of anti-neutrophil antibodies was first described by Lazerali in 1971 [6]. Currently, five human neutrophil antigens (HNA-1 to HNA-5) are included in the diagnostic procedure. In our case, anti-HNA-1 antibodies (FcγRIIIb receptor expressed only on neutrophils) were detected. HNA-1a and HNA-1b are the most common isoforms of this antigen [7]. The origin of the antibodies against HNA is unknown. Their synthesis may be associated with the phenomenon of molecular mimicry of infectious agents, especially parvovirus B19 (B19) [4]. The change of endogenous antigens may also be a consequence of taking medications, abnormal HLA antigen expression or dysfunctions of the immunosuppressive response [2]. The patient’s medical history should include questions about previous drug administration, symptoms of viral infections, e.g. Epstein-Barr virus (EBV), cytomegalovirus (CMV), B19, and history of hematologic/autoimmune diseases [8]. Interestingly, the count of neutrophils does not depend on the level of antibodies [5].

Spontaneous remission of neutropenia was observed in 95% of patients during 24 months of follow-up [4]. Treatment of AIN is individualized, depending on neutrophil levels, the age of the child, and the occurring infections. Due to the mild and self-limiting nature of the disease, routine antibiotic prophylaxis is not recommended. However, in some studies, antibiotic prophylaxis was beneficial for patients with recurrent infections, especially skin infections [9, 10]. The choice of therapy depends on the prevalence of specific bacteria and their resistance patterns in the environment [10]. Treatment of myeloid growth factors should be started after a previous bone marrow aspiration biopsy in children with severe infections or requiring surgical intervention [2]. High doses of intravenous immunoglobulin and corticosteroids may be effective in treating AIN in patients with life-threating infections. However, due to possible side effects, it is not standard treatment [5].

Conclusions

Autoimmune neutropenia of infancy, one of the most common causes of neutropenia, presents a diagnostic challenge in infants. Despite the benign course, serious infectious complications can occur. Due to numerous congenital anomalies and a lack of consent for an extended genetic test, the diagnosis of primary AIN in our patient will be finally confirmed after obtaining spontaneous remission of neutropenia.

Notes

[1] Conflicts of interest The authors declare no conflict of interest.

References

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2 

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3 

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6 

Lalezari P, Jiang AF, Yegen L, Santorineou M (1975): Chronic autoimmune neutropenia due to anti-NA2 antibody. N Engl J Med 293: 744-747.

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9 

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10 

Bruin M, Dassen A, Pajkrt D, et al. (2005): Primary autoimmune neutropenia in children: a study of neutrophil antibodies and clinical course. Vox Sang 88: 52-59.

Copyright: © 2021 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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