New Advances in the Study of CMTM6, a Focus on Its Novel Non-Canonical Cellular Locations, and Functions beyond Its Role as a PD-L1 Stabilizer
Abstract
:Simple Summary
Abstract
1. Introduction
2. Materials and Methods
2.1. Sample Collection and Preparation
2.2. Cell Culture
2.3. Isolation of Exosomes and Western Blot
2.4. ELISA
2.5. Immunofluorescence
2.6. Flow Cytometry
2.7. Statistical Analysis
3. Results
3.1. Plasma CMTM6 and PD-L1 Are Increased in Cervical Cancer
3.2. CMTM6 and PD-L1 Are Preferentially Released in Exosomes
3.3. CMTM6 and PD-L1 Are Present in CC-Derived Cell Line Lysates
3.4. CMTM6 Found in the Cell Membrane and Intracellularly in Cell Lines Derived from Cervical Cancer
3.5. PD-L1 Was Found in Its Typical Membrane-Associated Form in Cell Lines
3.6. CMTM6 Released by Cervical Cancer-Derived Cell Lines
4. Discussion
5. Conclusions
Supplementary Materials
Author Contributions
Funding
Institutional Review Board Statement
Informed Consent Statement
Data Availability Statement
Conflicts of Interest
References
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Healthy Donors | Cervical Cancer Patients | |
---|---|---|
(n = 23) | (n = 23) | |
Age | ||
Mean in years (range) | 45 (25–79) | 46 (25–72) |
Histopathology | ||
Squamous cell carcinoma | - | 12 (52%) |
Adenocarcinoma | - | 1 (4%) |
No information | - | 10 (44%) |
FIGO Stage | ||
I | 3 (13%) | |
II | 3 (13%) | |
III | 8 (35%) | |
IV | 5 (22%) | |
No information | 4 (17%) | |
Treatment scheme status | ||
Pre-treatment | - | 22 (96%) |
Post-treatment | - | 1 (4%) |
Chemotherapy | - | 1 (4%) |
Chemotherapy + Radiotherapy | - | 0 (0%) |
Disease free survival | - | 0 (0%) |
No information | 0 (0%) |
Healthy Donors | Cervical Cancer Patients | |
---|---|---|
(n = 11) | (n = 21) | |
Age | ||
Mean in years (range) | 43 (25–63) | 44 (25–79) |
Histopathology | ||
Squamous cell carcinoma | - | 13 (65%) |
Adenocarcinoma | - | 0 (0%) |
No information | - | 7 (35%) |
FIGO Stage | ||
I | 3 (14%) | |
II | 2 (10%) | |
III | 7 (33%) | |
IV | 5 (24%) | |
No information | 4 (19%) | |
Treatment scheme status | ||
Pre-treatment | - | 16 (76%) |
Post-treatment | - | 5 (24%) |
Chemotherapy | - | 1 (5%) |
Chemotherapy + Radiotherapy | - | 1 (5%) |
Disease free survival | - | 3 (14%) |
No information | - | 0 (0%) |
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Urciaga-Gutierrez, P.I.; Franco-Topete, R.A.; Bastidas-Ramirez, B.E.; Solorzano-Ibarra, F.; Rojas-Diaz, J.M.; Garcia-Barrientos, N.T.; Klimov-Kravtchenko, K.; Tellez-Bañuelos, M.C.; Ortiz-Lazareno, P.C.; Peralta-Zaragoza, O.; et al. New Advances in the Study of CMTM6, a Focus on Its Novel Non-Canonical Cellular Locations, and Functions beyond Its Role as a PD-L1 Stabilizer. Cancers 2024, 16, 3126. https://doi.org/10.3390/cancers16183126
Urciaga-Gutierrez PI, Franco-Topete RA, Bastidas-Ramirez BE, Solorzano-Ibarra F, Rojas-Diaz JM, Garcia-Barrientos NT, Klimov-Kravtchenko K, Tellez-Bañuelos MC, Ortiz-Lazareno PC, Peralta-Zaragoza O, et al. New Advances in the Study of CMTM6, a Focus on Its Novel Non-Canonical Cellular Locations, and Functions beyond Its Role as a PD-L1 Stabilizer. Cancers. 2024; 16(18):3126. https://doi.org/10.3390/cancers16183126
Chicago/Turabian StyleUrciaga-Gutierrez, Pedro Ivan, Ramon Antonio Franco-Topete, Blanca Estela Bastidas-Ramirez, Fabiola Solorzano-Ibarra, Jose Manuel Rojas-Diaz, Nadia Tatiana Garcia-Barrientos, Ksenia Klimov-Kravtchenko, Martha Cecilia Tellez-Bañuelos, Pablo Cesar Ortiz-Lazareno, Oscar Peralta-Zaragoza, and et al. 2024. "New Advances in the Study of CMTM6, a Focus on Its Novel Non-Canonical Cellular Locations, and Functions beyond Its Role as a PD-L1 Stabilizer" Cancers 16, no. 18: 3126. https://doi.org/10.3390/cancers16183126
APA StyleUrciaga-Gutierrez, P. I., Franco-Topete, R. A., Bastidas-Ramirez, B. E., Solorzano-Ibarra, F., Rojas-Diaz, J. M., Garcia-Barrientos, N. T., Klimov-Kravtchenko, K., Tellez-Bañuelos, M. C., Ortiz-Lazareno, P. C., Peralta-Zaragoza, O., Meneses-Acosta, A., Alejandre-Gonzalez, A. G., Bueno-Topete, M. R., Haramati, J., & del Toro-Arreola, S. (2024). New Advances in the Study of CMTM6, a Focus on Its Novel Non-Canonical Cellular Locations, and Functions beyond Its Role as a PD-L1 Stabilizer. Cancers, 16(18), 3126. https://doi.org/10.3390/cancers16183126