Correspondence to Dr Luregn J Schlapbach, Pediatric Intensive Care Unit, Department of Pediatrics, University of Bern, Inselspital, CH-3010 Bern, Switzerland; [email protected]

In a recent issue of Gut, Müller et al reported on excessive colitis in a murine model of mannan-binding lectin (MBL) deficiency.¹ They showed that absence of MBL can lead to uncontrolled intestinal inflammation detrimental to the host. MBL is a pattern-recognition molecule activating the complement system by the lectin pathway. H-ficolin is structurally closely related to MBL and can activate the lectin pathway of complement independently of MBL. While low levels of MBL occur in 10% of Caucasians, H-ficolin deficiency is extremely rare: studies involving over 100 000 adults found no case of H-ficolin deficiency, suggesting it exerts crucial functions for the human immune system.² The first report on the so far only patient diagnosed with H-ficolin deficiency was published only recently,³ describing a patient with repeated infections who presented with H-ficolin deficiency caused by homozygosity of the FCN3+1637delC frameshift mutation. With a gene frequency of 0.01, homozygosity is expected in 1 out of 10 000 individuals.³

Necrotising enterocolitis (NEC) is an overwhelming inflammatory disease typically occurring in premature neonates, characterised by...