To date, several types of early onset intractable diarrhea of infancy (IDI) have been recognized 12345678. Some of them involve primary epithelial abnormalities such as microvillous atrophy also called microvillous inclusion disease 5 and, more recently, intestinal epithelial dysplasia also called tufting enteropathy 67, while others are related to autoimmune disorders or complex syndromes involving mitochondrial disease or glycosylation proteins. The so-called "syndromic diarrhea" is an IDI syndrome associated with phenotypic abnormalities 9.

SD appears to be much less common than microvillous atrophy 57 or intestinal epithelial dysplasia 68. Many cases are not yet recognized since the description of this disorder is recent. To date, no epidemiological data are available. However, the prevalence can be estimated at around 1/300,000–400,000 live births in Western Europe. The largest cohort of patients has been reported at the Necker-Enfants Malades Hospital in Paris, France 9. The prevalence does not seem to differ significantly between ethnic groups. The disease seems to be more common in regions with a higher degree of consanguinity.

The patients present with diarrhea starting within the first 6 months of life (≤ 1 month in most cases). Severe malabsorption leads to early and severe protein energy malnutrition with failure to thrive and patients require parenteral nutrition (PN). Diarrhea persists while on bowel rest on PN. All affected infants have several features in common [Additional file 1]. They are small for gestional age (<10° percentile) and have an abnormal phenotype. All have facial dysmorphism with prominent forehead and cheeks, broad nasal root and hypertelorism (Figure 1). Most children have difficulties with fine motor movements and are mentally retarded. They have a distinct hair abnormality: woolly hair that is easily removed and poorly pigmented even in children of Middle Eastern origin. Microscopic analysis of the hair shaft reveals non-specific abnormalities: twisted hair (pili torti), aniso- and poilkilotrichosis, trichorrhexis nodosa and longitudinal breaks (Figure 2), and trichothiodystrophy. Some cases were reported with trichorrhexis blastysis under scanning electron microscopy 1011. In the same cases, biochemical analysis of hairs revealed several anomalies of the amino acid pattern, including a low cystine content in the cases of trichothiodystrophy. There is currently no specific biochemical profile. Around half of the patients have liver disease [Additional file 1].

Among the congenital forms of hair dysplasia, tricorrhexis nodosa (TN) is very common and can be present in several pathologic conditions 16171819. TN is the most common defect in the hair shaft, leading to hair breakage 20. The primary abnormality is a focal loss of cuticles, causing fraying of the cortical fibers 2122. As emphasized by Landers et al., TN may occur congenitally or can be acquired from chemical or physical trauma. Congenital TN has been associated with several syndromes including arginosuccinaciduria 23, citrullinemia 2425, Menkes syndrome 26, Netherton disease 2728, and syndromes associated with trichothiodystrophy hair shaft defect 29. SD patients have defective antibody responses despite normal serum immunoglobulin levels, and defective antigen-specific skin tests despite positive proliferative responses in vitro. The cause of this functional immune deficiency and of this severe protracted diarrhea is unknown. The relationship between low birth weight, dysmorphism, severe diarrhea, hair shaft defect, immune deficiency and neonatal hemochromatosis-like liver disease is unclear. The coexistence of morphological, trichological and immunological abnormalities with early-onset intractable diarrhea disproportionate to the mucosal architectural abnormality (consistent with a primary enterocyte abnormality) suggests either mutations within several genes, inherited together by linkage disequilibrium, or, more probably, interference with a higher level of control, such as a patterning gene as seen in the Netherton syndrome which is an autosomal recessive congenital ichthyosis featuring chronic inflammation of the skin, hair anomalies, epidermal hyperplasia with an impaired epidermal barrier function, failure to thrive and atopic manifestations. The disease is caused by mutations in the SPINK5 gene encoding the serine proteinase inhibitor lympho-epithelial Kazal-type inhibitor 3031. The characteristic hair abnormalities may allow a more focused search for candidate mutations, as relatively few genes have been implicated in hair development.

Diagnosis may be suspected early from the clinical presentation with the association of the following anomalies:

-intra-uterine growth retardation

-severe protracted diarrhea of early onset

-abnormal face with prominent forehead and cheeks

Most patients also have abnormal hair with tricorrhexis nodosa, immune deficiency, long-term growth failure and mental retardation in common. Liver disease is associated in about half of the patients and is variable in severity.

Early management consists of total parenteral nutrition (TPN) using central venous catheter in an experienced clinical setting. Patients usually have persistent diarrhea and, in enterally fed patients, malabsorption is severe. Its mechanisms are unknown, as villous atrophy is usually not as severe as the diarrhea is, and small bowel bacterial overgrowth or specific malabsorption have never been documented in these patients. Long-term PN is required for achieving growth even if catch up growth, in patients born SGA, cannot be achieved. Attempts at enteral feeding should be performed in all cases using semi-elemental diet or amino-acid formulas. Some patients will tolerate progressive increase of enteral feeding making them able to be weaned from PN. However, normal growth velocity is not always achieved on full enteral feeding. Course may vary according to the concomitant liver disease, the severity of the digestive disease and the occurrence of infections. It is well reflected by the reported cases [Additional file 1]. It is important to note that the liver disease is, in some cases, already present at onset of diarrhea and before diagnosis is established. In these cases, the liver disease is due to the disease rather than to the PN, suggesting that the PN should be carefully adapted according to the liver disease. Indeed, the associated liver disease may be worsened by a long-term inappropriate PN (continuous PN, lipid free, complicated by infections etc.) with rapid course to end-stage liver disease and patient death.

Finally, the prognosis of this type of intractable diarrhea of infancy is poor, with >25% of the currently reported patients who died between the ages of 2 and 5 years, some of them with early onset of cirrhosis. In the largest but oldest series, five of the eight children reported died within 5 years due to sepsis or cirrhosis, despite aggressive intervention 9. More recent case reports described better survival with long-term PN dependency or PN weaning in some cases 1112131415. In many patients, the severity of intestinal malabsorption and diarrhea makes them dependent on a daily long-term PN with subsequent risk of complications. However, it seems that some infants have milder phenotype with partial PN dependency or require only enteral feeding. In spite of adequate protein energy supplies, growth velocity remains low and final stature very short 911121314. Attempts with recombinant human growth hormone was used in one patient (data unpublished), but failed to improve growth and final stature. Most of the reported patients have intellectual deficiency of variable severity. Some were too young when they died to be thoroughly evaluated.

This very rare and heterogeneous syndrome has a poor prognosis with early death, liver cirrhosis or failure to thrive, and short stature with intellectual deficiency in the survivors. The heterogeneity of SD as well as the very different associated symptoms makes it very difficult to find an approach for understanding the genetic origin of the disease.

Prognosis has improved since the description of the first case with SD. Most patients now survive and about half of the patients may be weaned from PN at adolescence, but experience failure to thrive and final short stature.