Anchoring complex component laminin-5 and its subunits laminin (Ln)-alpha3 and
Ln-beta3 chains, Type VII collagen, and integrin chains alpha3, alpha6, and beta4
were studied in developing and adult human intestine and compared with findings on
Ln-alpha1 and Ln-alpha2 chains. In adult human duodenum, jejunum, and ileum, Ln-5
detected with a polyclonal antiserum and Ln-alpha3 and Ln-beta3 chains, detected with
monoclonal antibodies (MAbs), were restricted to the epithelial basement membranes
(BMs) of villi, whereas Ln-alpha2 chain was seen only focally in crypt bottoms. In
double labeling experiments, the stretch of crypt BM corresponding to the
proliferative cell compartment was found to be devoid of both Ln-alpha3 and Ln-alpha2
chains. Double labeling for Ln-5 and proliferating cell nuclear antigen also showed
an abrupt onset of Ln-5 expression exactly at the upper edge of the proliferative
cell compartment. Type VII collagen was negligible in duodenum and showed a rising
duodenal-ileal gradient localizing to villar BMs. Double labeling for Ln-5 and Type
VII collagen, however, indicated only partial co-distribution in the intestine.
Electron microscopy of ileum revealed both anchoring filaments and anchoring fibrils
but no hemidesmosomal plaques. Our results demonstrate the expression of Ln-5 in BMs
outside of stratified epithelia and indicate that Ln-5 in the intestine is associated
with the compartment of migrating and differentiating enterocytes. Absence of
hemidesmosomes and the presence of other anchoring complex components, such as Ln-5,
Type VII collagen, and integrin chains alpha3, alpha6, and beta4, suggests unique
properties for epithelial cell attachment in the intestine.