Genomic diagnosis and multisystem phenotyping in pediatric congenital analbuminemia: clinical, coagulation, and immune signatures

SEFER ARINÇ, ASENA; Altunbas, Melek; ERMAN, BARAN; Can, Salim; Bulutoglu, Alper; Hubrack, Satanay; Ford, Katherine; Makhlouf, Melanie; Saraiva, Luis; ÖNDER, GİZEM; HATIRNAZ NG, ÖZDEN; Usta, Ayse; Guller, Dilek; Baser, Dilek; Akgun, Gamze; Aba, Umran; Erdogan, Rahmi; BEŞER, ÖMER; Cokugras, Fugen; Ar, Fatma; Urganci, Nafiye; Dincer, Oguz; BİLGİÇ ELTAN, SEVGİ; BARIŞ, SAFA; AYDINER, ELİF; Lo, Bernice; Ozen, Ahmet

doi:10.3389/fped.2026.1810945

Genomic diagnosis and multisystem phenotyping in pediatric congenital analbuminemia: clinical, coagulation, and immune signatures

SEFER ARINÇ A. P., Altunbas M. Y., ERMAN B., Can S., Bulutoglu A., Hubrack S., ...Daha Fazla

FRONTIERS IN PEDIATRICS, cilt.14, 2026 (SCI-Expanded, Scopus)

Yayın Türü: Makale / Tam Makale
Cilt numarası: 14
Basım Tarihi: 2026
Doi Numarası: 10.3389/fped.2026.1810945
Dergi Adı: FRONTIERS IN PEDIATRICS
Derginin Tarandığı İndeksler: Science Citation Index Expanded (SCI-EXPANDED), Scopus, EMBASE, Directory of Open Access Journals
Açık Arşiv Koleksiyonu: AVESİS Açık Erişim Koleksiyonu
Recep Tayyip Erdoğan Üniversitesi Adresli: Evet

Özet

Background: Congenital analbuminemia (CAA) is an ultrarare autosomal recessive disorder caused by biallelic pathogenic variants in the ALB gene, leading to absent or severely reduced serum albumin. Although historically considered a benign biochemical condition, emerging evidence suggests that pediatric CAA may be associated with clinically relevant multisystem manifestations. Methods: We conducted a longitudinal integrative study involving five children from two kindreds, all with genetically confirmed CAA. Their clinical features were thoroughly documented, along with extended coagulation tests and immunological profiling. Results: All patients presented with persistent hypoalbuminemia, early-onset edema, gastrointestinal morbidity (frequently leading to misdiagnosis as protein-losing enteropathy), antenatal complications, recurrent respiratory infections, and dyslipidemia. Genetic testing revealed an ALB splice-site mutation (c.1428 + 2T > C) in one kindred and a novel homozygous frameshift insertion (p.Glu69Ter) in the second. Coagulation profiling identified a reproducible prothrombotic signature, including elevated fibrinogen, D-dimer, and strikingly increased FXI activity, with one patient suffering life-threatening cerebral thrombosis. Immunological evaluation demonstrated preserved leukocyte and lymphocyte counts, preserved or elevated IgG levels, variable antigen-specific vaccine responses, reduced kappa-deleting recombination excision circle values in the tested patients, and skewing of CD4(+) T cells toward effector memory subsets, consistent with immune dysregulation rather than frank immunodeficiency. Conclusions: This study provides detailed multisystem phenotyping of pediatric CAA and supports the view that CAA may present with clinically relevant gastrointestinal, metabolic, infectious, and hemostatic manifestations beyond isolated hypoalbuminemia. Early molecular diagnosis may reduce unnecessary invasive investigations and facilitate individualized monitoring for infectious and thrombotic complications. Larger multicenter studies with longitudinal follow-up and functional validation are required to confirm these findings.