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. 2023 Mar 28;20:22. doi: 10.1186/s12987-023-00424-5

Table 5.

The reported pathogenic missense mutations in other classic CLDNs

Identified mutation Position in CLDN-5 Homology level Estimated or validated changes Ref.
CLDN-1 (R81H) R81 Very High Mis-localization due to the structural instability [144]
CLDN-2 (G161R) G161 Very high In silico docking study indicates it may affect oligomer formations [233]
CLDN-9 (E159K) E159 Very High

Incorporation into the TJs or barrier-forming ability were not impaired.

But this position needs for cis-interaction

[234]
CLDN-10a (R78G) R81 Very High Mis-localization due to the structural instability [143]
CLDN-10b (N48K) G48 High TJs were not formed correctly due to the disturbance of classic CLDN signature [235]
CLDN-10b (D73N) S74 Low Incorporation into the TJs was partially impaired by attenuation of CLDN-10b specific intra-molecule interaction [148, 236]
CLDN-10b (P149R) P150 Very High Incorporation into the TJs was partially impaired by impaired cis-oligomerization
CLDN-10b (S131L) A132 Low Mis-localization [237]

CLDN-10b

(G165A)

G167 Very high Incorporation into the TJs was partially impaired and trans-interaction ability was clearly attenuated [238]
CLDN-14 (V85D) V85 High Mis-localization [239]
CLDN-14 (G101R) G101 Very high It localized at the cell border, but TJs were not formed correctly
CLDN-14 (R81H) R81 Very High Mis-localization due to the structural instability [145]
CLDN-19 (Q57E) Q57 High Mis-localization [161]
CLDN-19 (G20D) G20 High Mis-localization
CLDN-19 (L90P) L90 High Incorporation into the TJs was not impaired but its function was partially impaired.
CLDN-19 (G123R) G122 Very high Incorporation into the TJs was not impaired but its function was partially impaired.