Abstract
Development of the brain ventricular system of vertebrates and the molecular mechanisms involved are not fully understood. The developmental genes expressed in the elements of the brain ventricular system such as the ependyma and circumventricular organs act as molecular determinants of cell adhesion critical for the formation of brain ventricular system. They control brain development and function, including the flow of cerebrospinal fluid. Here, we describe the novel distantly related member of the zebrafish L1-CAM family of genes—camel. Whereas its maternal transcripts distributed uniformly, the zygotic transcripts demonstrate clearly defined expression patterns, in particular in the axial structures: floor plate, hypochord, and roof plate. camel expresses in several other cell lineages with access to the brain ventricular system, including the midbrain roof plate, subcommissural organ, organum vasculosum lamina terminalis, median eminence, paraventricular organ, flexural organ, and inter-rhombomeric boundaries. This expression pattern suggests a role of Camel in neural development. Several isoforms of Camel generated by differential splicing of exons encoding the sixth fibronectin type III domain enhance cell adhesion differentially. The antisense oligomer morpholino-mediated loss-of-function of Camel affects cell adhesion and causes hydrocephalus and scoliosis manifested via the tail curled down phenotype. The subcommissural organ’s derivative—the Reissner fiber—participates in the flow of cerebrospinal fluid. The Reissner fiber fails to form upon morpholino-mediated Camel loss-of-function. The Camel mRNA–mediated gain-of-function causes the Reissner fiber misdirection. This study revealed a link between Chl1a/Camel and Reissner fiber formation, and this supports the idea that CHL1 is one of the scoliosis factors.
Highlights
The subcommissural organ (SCO) is an ependymal brain gland found in the diencephalic roof of the third ventricle at the entrance to the cerebral aqueduct
Chl1 has been suggested as a susceptibility gene of adolescent idiopathic scoliosis in humans (Sharma et al 2011), other studies failed to support this link (Qiu et al 2014)
In the species, where a pair of ohnologs exists, the chl1 genes must be renamed reciprocally similar to many other ohnologs that were misnamed as suggested by the evolution-based systematic synteny analysis
Summary
The subcommissural organ (SCO) is an ependymal brain gland found in the diencephalic roof of the third ventricle at the entrance to the cerebral aqueduct. Several genes or regulators of axial midline structures including, but not limited to, the genes of the nodal and hedgehog signaling pathways (Roelink et al 1994; Higashijima et al 1997; Sampath et al 1998; Lehmann and Naumann 2005) control the formation and function of cells that generate the RF such as the SCO (Sterba 1969; Oksche 1969), flexural organ (FO) (Olsson 1958), and floor plate (FP) (Rodríguez et al 1996). RF formation takes place by polymerization of SCO-spondin and depends on additional agents
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