Evaluation of Immunohistochemical Expression of ALK-1 in Gliomas, WHO Grade 4 and Its Correlation with IDH1-R132H Mutation Status.
Rasha Ahmed KhairyEman Mohamed MomtazAhmed Mahmoud Abd El AzizPassant Essam Eldin ShibelPublished in: Asian Pacific journal of cancer prevention : APJCP (2024)
ALK-1 immunoexpression was detected in 22.9% of our cases and IDH1-R132H mutation was detected in 12.9% of them. ALK-1 expression (100%) was only detected in the more aggressive IDH R132H-negative GBs. ALK-1 expression was also noted in the larger-sized tumors, more in males and patients older than the mean age. Conclusion: Our results suggest that mutations in ALK-1 may predict a more dismal prognosis since ALK expression was only noted in IDH-R132H negative GBs known to have a considerably poorer outcome compared to IDH-R132H mutant cases. GBs with detectable ALK-protein expression could potentially experience substantial clinical advantages through the utilization of newly introduced ALK inhibitors allowing personalized treatment to a subset of patients. Hence, future studies targeting ALK in IDH wildtype Glioblastomas including clinical trials on larger scales are recommended.
Keyphrases
- advanced non small cell lung cancer
- poor prognosis
- low grade
- end stage renal disease
- wild type
- clinical trial
- ejection fraction
- newly diagnosed
- chronic kidney disease
- peritoneal dialysis
- epidermal growth factor receptor
- high grade
- prognostic factors
- binding protein
- randomized controlled trial
- drug delivery
- current status
- patient reported outcomes
- open label
- combination therapy
- patient reported
- cancer therapy
- double blind