Surfactant proteins (SFTPs) are trafficked from the ER membr...
| created | [InstanceEdit:5688355] Jassal, Bijay, 2015-04-16 |
| dbId | 5688368 |
| displayName | Surfactant proteins (SFTPs) are trafficked from the ER membr... |
| modified | [InstanceEdit:6791022] Jassal, Bijay, 2015-08-17 |
| schemaClass | Summation |
| text | Surfactant proteins (SFTPs) are trafficked from the ER membrane to lamellar bodies (LBs) via the multi-vesicle body (MVB). The pro-SFTPs B and C are cleaved here to produce functional SFTPs. Defects in the SFTPC gene result in protein misfolding, misrouting and/or misprocessing resulting in accumulation of partially-processed, inactive pro-SFTPC in alveoli causing cell toxicity. Defects in SFTPC can cause pulmonary surfactant metabolism dysfunction 2 (SMDP2; MIM:610913), a rare lung disorder due to impaired surfactant homeostasis characterised by alveoli filling with floccular material. Cellular responses to the misfolded pro-SFTPC products include ER stress, the activation of reactive oxygen species and autophagy. Excessive lipoprotein accumulation in the alveoli results in a form of respiratory distress syndrome in premature infants (RDS; MIM:267450). Mutations causing RDS that arrest the pro-protein in the ER include P30L and P115L (Thurm et al. 2013). |
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