Lysosomal chloride transporter CLH-6 protects lysosome membrane integrity via cathepsin activation

Lysosomal integrity is vital for cell homeostasis, but the underlying mechanisms are poorly understood. Here, we identify CLH-6, the C. elegans ortholog of the lysosomal Cl-/H+ antiporter ClC-7, as an important factor for protecting lysosomal integrity. Loss of CLH-6 affects lysosomal degradation, causing cargo accumulation and membrane rupture. Reducing cargo delivery or increasing CPL-1/cathepsin L or CPR-2/cathepsin B expression suppresses these lysosomal defects. Inactivation of CPL-1 or CPR-2, like CLH-6 inactivation, affects cargo digestion and causes lysosomal membrane rupture. Thus, loss of CLH-6 impairs cargo degradation, leading to membrane damage of lysosomes. In clh-6(lf) mutants, lysosomes are acidified as in wild type but contain lower chloride levels, and cathepsin B and L activities are significantly reduced. Cl- binds to CPL-1 and CPR-2 in vitro, and Cl- supplementation increases lysosomal cathepsin B and L activities. Altogether, these findings suggest that CLH-6 maintains the luminal chloride levels required for cathepsin activity, thus facilitating substrate digestion to protect lysosomal membrane integrity. Zhang et al. identify the lysosomal Cl-/H+ antiporter CLH-6/ClC-7 as an important factor for protecting lysosome integrity. They reveal that CLH-6 maintains the luminal chloride levels required for cathepsin activity, thus facilitating substrate digestion to preserve lysosomal membrane stability.

Automated summary

CLH-6 is identified as an important factor for protecting lysosomal integrity in C. elegans. Loss of CLH-6 impairs cargo degradation and leads to lysosomal membrane damage. Maintaining luminal chloride levels is crucial for cathepsin activity and preserving lysosomal membrane stability.