Abstract
ObjectivesComplete C6 deficiency (C6Q0) is a rare primary immunodeficiency leading to increased susceptibility to recurrent Neisseria infections. Patients with C6Q0 have mostly been reported in individuals of African ancestry previously, but never in Chinese. We identify the first Chinese patients with C6Q0 through family screening of an index case presenting with recurrent Neisseria meningitis with septicaemia and performed extensive clinical, serological and genetic investigations.MethodsTwo variants in C6 were identified by next‐generation sequencing and confirmed by Sanger sequencing in an index case of C6Q0. Immunological investigations, complement haemolytic assays (CH50/AH50), C6 gene sequencing and quantification of serum C6 levels were performed for all available members of his nonconsanguineous family.ResultsThree C6Q0 patients were identified with near‐absent C6 levels, absent CH50/AH50 activity and compound heterozygous for two nonsense mutations in the C6 gene: NM_000065.4:c.1786C>T (p.Arg596Ter) and NM_000065.4:c.1816C>T (p.Arg606Ter). Neither mutations have been reported to be pathogenic previously. Two other family members who were heterozygous for either p.Arg596Ter or and p.Arg606Ter had intermediate C6 levels but preserved CH50/AH50 activity. These two loss‐of‐function mutations showed a strong genotype–phenotype correlation in C6 levels.ConclusionsWe report on two compound heterozygous mutations in C6, p.Arg596Ter and p.Arg606Ter inherited in three patients of the first recorded Chinese pedigree of C6Q0. Neither mutations had been reported to be pathogenic previously. We demonstrate that heterozygous family members with subtotal C6 levels had preserved complement haemolytic function and demonstrate a threshold effect of C6 protein level.
Highlights
Human complement component C6 is one of the essential terminal complement components (TCC) and is crucial for assembly of the membrane attack complex responsible for osmotic lysis of susceptible cells.[1]
We identified the first Chinese patients with C6Q0 through family screening of an index case presenting with recurrent Neisseria meningitis with septicaemia
We describe the first Chinese pedigree of C6Q0 with two mutations, p.Arg596Ter and p.Arg606Ter, neither of which had been reported to be pathogenic previously
Summary
Human complement component C6 is one of the essential terminal complement components (TCC) and is crucial for assembly of the membrane attack complex responsible for osmotic lysis of susceptible cells.[1]. Patients with C6 deficiency (OMIM: 612446) are categorised functionally into subtotal (C6SD) or complete [ known as quantitatively zero (C6Q0)].2. Similar to other TCC deficiencies, C6Q0 is a primary immunodeficiency (PID) characterised by increased susceptibility to Neisseria spp.[1,3–5]. C6Q0 is an autosomal recessive PID, and patients suffer from significantly more serious illness or death as sequelae from recurrent meningococcal episodes.[7]. As < 10% of normal C6 is required for sufficient complement activity, C6SD is not associated with meningococcal disease and has even been postulated to possibly confer evolutionary benefit by reduced antimicrobial activity but less severe endotoxin shock.[8,9]
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