TY - JOUR
T1 - Paranodal permeability in "myelin mutants"
AU - Shroff, Seema
AU - Mierzwa, Amanda
AU - Scherer, Steven S.
AU - Peles, Elior
AU - Arevalo, Juan C.
AU - Chao, Moses V.
AU - Rosenbluth, Jack
N1 - NIH [NS 37475, NS50220, HD23315, NS21072, NS43174]; National Multiple Sclerosis Society [RG 3618]; Israeli Academy of SciencesGrant sponsor: Supported by grants NS 37475 from the NIH and RG 3618 from the National Multiple Sclerosis Society to JR, NIH grants NS50220 and the Israeli Academy of Sciences to EP, NIH grants HD23315 and NS21072 to MC and NS43174 to SSS. E. P. is the Incumbent of the Hanna Hertz Professorial Chair for Multiple Sclerosis and Neuroscience.
PY - 2011/10
Y1 - 2011/10
N2 - Fluorescent dextran tracers of varying sizes have been used to assess paranodal permeability in myelinated sciatic nerve fibers from control and three "myelin mutant" mice, Caspr-null, cst-null, and shaking. We demonstrate that in all of these the paranode is permeable to small tracers (3 kDa and 10 kDa), which penetrate most fibers, and to larger tracers (40 kDa and 70 kDa), which penetrate far fewer fibers and move shorter distances over longer periods of time. Despite gross diminution in transverse bands (TBs) in the Caspr-null and cst-null mice, the permeability of their paranodal junctions is equivalent to that in controls. Thus, deficiency of TBs in these mutants does not increase the permeability of their paranodal junctions to the dextrans we used, moving from the perinodal space through the paranode to the internodal periaxonal space. In addition, we show that the shaking mice, which have thinner myelin and shorter paranodes, show increased permeability to the same tracers despite the presence of TBs. We conclude that the extent of penetration of these tracers does not depend on the presence or absence of TBs but does depend on the length of the paranode and, in turn, on the length of "pathway 3," the helical extracellular pathway that passes through the paranode parallel to the lateral edge of the myelin sheath.
AB - Fluorescent dextran tracers of varying sizes have been used to assess paranodal permeability in myelinated sciatic nerve fibers from control and three "myelin mutant" mice, Caspr-null, cst-null, and shaking. We demonstrate that in all of these the paranode is permeable to small tracers (3 kDa and 10 kDa), which penetrate most fibers, and to larger tracers (40 kDa and 70 kDa), which penetrate far fewer fibers and move shorter distances over longer periods of time. Despite gross diminution in transverse bands (TBs) in the Caspr-null and cst-null mice, the permeability of their paranodal junctions is equivalent to that in controls. Thus, deficiency of TBs in these mutants does not increase the permeability of their paranodal junctions to the dextrans we used, moving from the perinodal space through the paranode to the internodal periaxonal space. In addition, we show that the shaking mice, which have thinner myelin and shorter paranodes, show increased permeability to the same tracers despite the presence of TBs. We conclude that the extent of penetration of these tracers does not depend on the presence or absence of TBs but does depend on the length of the paranode and, in turn, on the length of "pathway 3," the helical extracellular pathway that passes through the paranode parallel to the lateral edge of the myelin sheath.
UR - http://www.scopus.com/inward/record.url?scp=79960702238&partnerID=8YFLogxK
U2 - https://doi.org/10.1002/glia.21188
DO - https://doi.org/10.1002/glia.21188
M3 - مقالة
SN - 0894-1491
VL - 59
SP - 1447
EP - 1457
JO - GLIA
JF - GLIA
IS - 10
ER -