Editorial - T790M mutation and clinical outcomes with genuine osimertinib
CC BY-NC-ND 4.0 · Indian J Med Paediatr Oncol 2019; 40(01): 7-8
DOI: DOI: 10.4103/ijmpo.ijmpo_40_19
The tyrosine kinase inhibitor (TKI) revolution, in the management of lung cancer, is now more than 10 years old.[1] The insight that molecular testing and identification of driver mutations is key to the selection of the right treatment is also well established and led to the era of precision medicine and personalized therapy. It also led to the recognition that there were significant geographic and ethnic variations in the incidence of epidermal growth factor receptor (EGFR) mutations.[2] Suddenly, our patients with lung cancer had a bouquet of options that would give them longer survival and better quality of life.[3] Accumulation of cumulative data and improvement in laboratory techniques refined our understanding and threw up new questions.[4] We also noted the experience with imatinib and chronic myeloid leukemia being replicated in lung cancer as well.[5] Patients who responded well to initial treatment of gefitinib invariably develop progressive disease.[6]
The specific mutation T790M was quickly recognized as the main reason for progression in patients with lung cancers who had presented with EGFR mutation and were treated with oral first-generation TKIs.[6] Availability of second- and third-generation TKIs rekindled hope.[7] Both afatinib and osimertinib quickly gained a prominent place in the management of EGFR-mutated lung cancer. The AURA3 trial showed that in T790M mutation-positive advanced lung cancer, osimertinib provided median progression-free survival (PFS) of 10.1 months as compared to 4.4 months with platinum-pemetrexed combination chemotherapy.[6] The first Indian report of 13 patients showed good symptom control as well as an overall response rate of 55% (6/11 evaluable patients).[8] This was comparable to the objective response rate to osimertinib of 71% in AURA3.[6]
This issue of IJMPO presents prospective observational data on 90 patients who had progressive disease while on EGFR TKI.[9] They were evaluated by molecular testing on rebiopsy or ctDNA for T790M mutations, which were detected in 52.2% (47/90 patients). T790M mutation was identified on repeat tissue biopsy in 82.9% (39/47) and with CTDNA in 17% (8/47). For the whole group, at progression, biopsy was feasible in 77/90 (85%) patients.[10] Interestingly, the incidence of T790M mutation was similar in tissue (50.6%) and liquid biopsy (52.9%), giving the reassurance that liquid biopsy is robust enough to be relied upon for clinical decisions.
Among the T790M-mutated patients with progressive disease, 46 could be commenced on osimertinib. At 15-month follow-up, the overall response rate and median PFS were 65.21% and 12.45 months, respectively. The median overall survival was not reached (67.3%; 33/46 patients being alive in the osimertinib cohort). There was also no therapy discontinuation related to adverse effects. This is encouraging news for our patients with lung cancer. Several years of survival with good quality of life is possible by judicious sequencing of therapy. Surrogate markers to fine tune the decision-making process further will be beneficial. The authors have identified that PFS was significantly better with second-line osimertinib if patients had achieved a complete response to first-line oral TKI therapy.
However, there are certain unscrupulous businesses and people, who are fooling lung cancer patients in India with the promise of cheap TKIs - at a fraction of the cost of the original genuine medicine.[11] We have previously described how our patients are becoming victims of fake, illegal “generic medicines” made available in the grey market without bill, without approval by the Drug Controller General of India, without any testing in the laboratory or humans, from across our borders and without even the permission to market or sell in their own country. This is a scam allegedly of value of 500 crore rupees every month! Our patients' lives are being put at risk by being sold attractively packaged smart looking plastic containers with seemingly authentic labels whose contents have not been tested by any regulatory authority anywhere in the world. Unless our lung cancer patients are alert, they will continue to deteriorate while consuming material that at best is placebo and could potentially contain chemicals or impurities that could put their lives at immediate risk. Under the circumstances, how can we provide them with the benefit of genuine medicines and the improved response, survival, and quality of life that have been proven with the use of genuine official TKIs?
Publication History
Article published online:
08 June 2021
© 2019. Indian Society of Medical and Paediatric Oncology. This is an open access article published by Thieme under the terms of the Creative Commons Attribution-NonDerivative-NonCommercial-License, permitting copying and reproduction so long as the original work is given appropriate credit. Contents may not be used for commercial purposes, or adapted, remixed, transformed or built upon. (https://creativecommons.org/licenses/by-nc-nd/4.0/).
Thieme Medical and Scientific Publishers Pvt. Ltd.
A-12, 2nd Floor, Sector 2, Noida-201301 UP, India
The tyrosine kinase inhibitor (TKI) revolution, in the management of lung cancer, is now more than 10 years old.[1] The insight that molecular testing and identification of driver mutations is key to the selection of the right treatment is also well established and led to the era of precision medicine and personalized therapy. It also led to the recognition that there were significant geographic and ethnic variations in the incidence of epidermal growth factor receptor (EGFR) mutations.[2] Suddenly, our patients with lung cancer had a bouquet of options that would give them longer survival and better quality of life.[3] Accumulation of cumulative data and improvement in laboratory techniques refined our understanding and threw up new questions.[4] We also noted the experience with imatinib and chronic myeloid leukemia being replicated in lung cancer as well.[5] Patients who responded well to initial treatment of gefitinib invariably develop progressive disease.[6]
The specific mutation T790M was quickly recognized as the main reason for progression in patients with lung cancers who had presented with EGFR mutation and were treated with oral first-generation TKIs.[6] Availability of second- and third-generation TKIs rekindled hope.[7] Both afatinib and osimertinib quickly gained a prominent place in the management of EGFR-mutated lung cancer. The AURA3 trial showed that in T790M mutation-positive advanced lung cancer, osimertinib provided median progression-free survival (PFS) of 10.1 months as compared to 4.4 months with platinum-pemetrexed combination chemotherapy.[6] The first Indian report of 13 patients showed good symptom control as well as an overall response rate of 55% (6/11 evaluable patients).[8] This was comparable to the objective response rate to osimertinib of 71% in AURA3.[6]
This issue of IJMPO presents prospective observational data on 90 patients who had progressive disease while on EGFR TKI.[9] They were evaluated by molecular testing on rebiopsy or ctDNA for T790M mutations, which were detected in 52.2% (47/90 patients). T790M mutation was identified on repeat tissue biopsy in 82.9% (39/47) and with CTDNA in 17% (8/47). For the whole group, at progression, biopsy was feasible in 77/90 (85%) patients.[10] Interestingly, the incidence of T790M mutation was similar in tissue (50.6%) and liquid biopsy (52.9%), giving the reassurance that liquid biopsy is robust enough to be relied upon for clinical decisions.
Among the T790M-mutated patients with progressive disease, 46 could be commenced on osimertinib. At 15-month follow-up, the overall response rate and median PFS were 65.21% and 12.45 months, respectively. The median overall survival was not reached (67.3%; 33/46 patients being alive in the osimertinib cohort). There was also no therapy discontinuation related to adverse effects. This is encouraging news for our patients with lung cancer. Several years of survival with good quality of life is possible by judicious sequencing of therapy. Surrogate markers to fine tune the decision-making process further will be beneficial. The authors have identified that PFS was significantly better with second-line osimertinib if patients had achieved a complete response to first-line oral TKI therapy.
However, there are certain unscrupulous businesses and people, who are fooling lung cancer patients in India with the promise of cheap TKIs - at a fraction of the cost of the original genuine medicine.[11] We have previously described how our patients are becoming victims of fake, illegal “generic medicines” made available in the grey market without bill, without approval by the Drug Controller General of India, without any testing in the laboratory or humans, from across our borders and without even the permission to market or sell in their own country. This is a scam allegedly of value of 500 crore rupees every month! Our patients' lives are being put at risk by being sold attractively packaged smart looking plastic containers with seemingly authentic labels whose contents have not been tested by any regulatory authority anywhere in the world. Unless our lung cancer patients are alert, they will continue to deteriorate while consuming material that at best is placebo and could potentially contain chemicals or impurities that could put their lives at immediate risk. Under the circumstances, how can we provide them with the benefit of genuine medicines and the improved response, survival, and quality of life that have been proven with the use of genuine official TKIs?
Conflict of Interest
There are no conflicts of interest.
- Parikh P, Chang AN, Nag S, Digumarti R, Bhattacharyya GS, Doval DC. et al. Clinical experience with gefitinib in Indian patients. J Thorac Oncol 2008; 3: 380-5
- Parikh P, Puri T. Personalized medicine: Lung cancer leads the way. Indian J Cancer 2013; 50: 77-9
- Parikh PM, Ranade AA, Govind B, Ghadyalpatil N, Singh R, Bharath R. et al. Lung cancer in India: Current status and promising strategies. South Asian J Cancer 2016; 5: 93-5
- Prabhash D, Parikh PM, Rajappa SJ, Noronha V, Joshi A, Aggarwal S. et al. Patterns of epidermal growth factor receptor testing across 111 tertiary care centers in India: Result of a questionnaire-based survey. South Asian J Cancer 2018; 7: 203-6
- Malhotra H, Sharma P, Malhotra B, Bhargava S, Jasuja S, Kumar M. et al. Molecular response to imatinib & its correlation with mRNA expression levels of imatinib influx & efflux transporters in patients with chronic myeloid leukaemia in chronic phase. Indian J Med Res 2015; 376: 175-82
- Mok TS, Wu TL, Ahn MJ, Garassino MC, Kim HR, Ramalingam SS. et al. Osimertinib or platinum-pemetrexed in EGFR T790M-positive lung cancer. N Engl J Med 2017; 376: 629-40
- Batra U, Lokeshwar N, Gupta S, Shirsath P. Role of epidermal growth factor receptor-tyrosine kinase inhibitors in the management of central nervous system metastases in epidermal growth factor receptor mutation-positive nonsmall cell lung cancer patients. Indian J Cancer 2017; 54: S37-S44
- Noronha V, Majumdar S, Joshi A, Patil V, Trivedi V, Chougule A. et al. Osimertinib in Indian patients with T790M-positive advanced nonsmall cell lung cancer. South Asian J Cancer 2017; 6: 143
- Jaiswal R, Pinninti R, Mohan MV, Santa A, Boyella PK, Nambaru L. et al. T790M mutation and clinical outcomes with osimertinib in patients with epidermal growth factor receptormutant nonsmall cell lung cancer. Indian J Med Paediatr Oncol 2019; 40: 73-8
- Zanwar S, Noronha V, Joshi A, Patil VM, Chougule A, Kumar R. et al. Repeat biopsy in epidermal growth factor receptor mutation-positive nonsmall cell lung cancer: Feasibility, limitations, and clinical utility in Indian patients. Indian J Cancer 2017; 54: 280-4
- Parikh PM, Bhattacharyya GS, Hingmire SS, Mehta P, Rangrajan B, Natrajan G. Our patient at risk from unauthorized, unapproved, illegally imported fake “generic medicines”. Indian J Med Sci 2018; 70: 43-7
Address for correspondence
Publication History
Article published online:
08 June 2021
© 2019. Indian Society of Medical and Paediatric Oncology. This is an open access article published by Thieme under the terms of the Creative Commons Attribution-NonDerivative-NonCommercial-License, permitting copying and reproduction so long as the original work is given appropriate credit. Contents may not be used for commercial purposes, or adapted, remixed, transformed or built upon. (https://creativecommons.org/licenses/by-nc-nd/4.0/).
Thieme Medical and Scientific Publishers Pvt. Ltd.
A-12, 2nd Floor, Sector 2, Noida-201301 UP, India
- 1 Parikh P, Chang AN, Nag S, Digumarti R, Bhattacharyya GS, Doval DC. et al. Clinical experience with gefitinib in Indian patients. J Thorac Oncol 2008; 3: 380-5
- 2 Parikh P, Puri T. Personalized medicine: Lung cancer leads the way. Indian J Cancer 2013; 50: 77-9
- 3 Parikh PM, Ranade AA, Govind B, Ghadyalpatil N, Singh R, Bharath R. et al. Lung cancer in India: Current status and promising strategies. South Asian J Cancer 2016; 5: 93-5
- 4 Prabhash D, Parikh PM, Rajappa SJ, Noronha V, Joshi A, Aggarwal S. et al. Patterns of epidermal growth factor receptor testing across 111 tertiary care centers in India: Result of a questionnaire-based survey. South Asian J Cancer 2018; 7: 203-6
- 5 Malhotra H, Sharma P, Malhotra B, Bhargava S, Jasuja S, Kumar M. et al. Molecular response to imatinib & its correlation with mRNA expression levels of imatinib influx & efflux transporters in patients with chronic myeloid leukaemia in chronic phase. Indian J Med Res 2015; 376: 175-82
- 6 Mok TS, Wu TL, Ahn MJ, Garassino MC, Kim HR, Ramalingam SS. et al. Osimertinib or platinum-pemetrexed in EGFR T790M-positive lung cancer. N Engl J Med 2017; 376: 629-40
- 7 Batra U, Lokeshwar N, Gupta S, Shirsath P. Role of epidermal growth factor receptor-tyrosine kinase inhibitors in the management of central nervous system metastases in epidermal growth factor receptor mutation-positive nonsmall cell lung cancer patients. Indian J Cancer 2017; 54: S37-S44
- 8 Noronha V, Majumdar S, Joshi A, Patil V, Trivedi V, Chougule A. et al. Osimertinib in Indian patients with T790M-positive advanced nonsmall cell lung cancer. South Asian J Cancer 2017; 6: 143
- 9 Jaiswal R, Pinninti R, Mohan MV, Santa A, Boyella PK, Nambaru L. et al. T790M mutation and clinical outcomes with osimertinib in patients with epidermal growth factor receptormutant nonsmall cell lung cancer. Indian J Med Paediatr Oncol 2019; 40: 73-8
- 10 Zanwar S, Noronha V, Joshi A, Patil VM, Chougule A, Kumar R. et al. Repeat biopsy in epidermal growth factor receptor mutation-positive nonsmall cell lung cancer: Feasibility, limitations, and clinical utility in Indian patients. Indian J Cancer 2017; 54: 280-4
- 11 Parikh PM, Bhattacharyya GS, Hingmire SS, Mehta P, Rangrajan B, Natrajan G. Our patient at risk from unauthorized, unapproved, illegally imported fake “generic medicines”. Indian J Med Sci 2018; 70: 43-7
References
- Parikh P, Chang AN, Nag S, Digumarti R, Bhattacharyya GS, Doval DC. et al. Clinical experience with gefitinib in Indian patients. J Thorac Oncol 2008; 3: 380-5
- Parikh P, Puri T. Personalized medicine: Lung cancer leads the way. Indian J Cancer 2013; 50: 77-9
- Parikh PM, Ranade AA, Govind B, Ghadyalpatil N, Singh R, Bharath R. et al. Lung cancer in India: Current status and promising strategies. South Asian J Cancer 2016; 5: 93-5
- Prabhash D, Parikh PM, Rajappa SJ, Noronha V, Joshi A, Aggarwal S. et al. Patterns of epidermal growth factor receptor testing across 111 tertiary care centers in India: Result of a questionnaire-based survey. South Asian J Cancer 2018; 7: 203-6
- Malhotra H, Sharma P, Malhotra B, Bhargava S, Jasuja S, Kumar M. et al. Molecular response to imatinib & its correlation with mRNA expression levels of imatinib influx & efflux transporters in patients with chronic myeloid leukaemia in chronic phase. Indian J Med Res 2015; 376: 175-82
- Mok TS, Wu TL, Ahn MJ, Garassino MC, Kim HR, Ramalingam SS. et al. Osimertinib or platinum-pemetrexed in EGFR T790M-positive lung cancer. N Engl J Med 2017; 376: 629-40
- Batra U, Lokeshwar N, Gupta S, Shirsath P. Role of epidermal growth factor receptor-tyrosine kinase inhibitors in the management of central nervous system metastases in epidermal growth factor receptor mutation-positive nonsmall cell lung cancer patients. Indian J Cancer 2017; 54: S37-S44
- Noronha V, Majumdar S, Joshi A, Patil V, Trivedi V, Chougule A. et al. Osimertinib in Indian patients with T790M-positive advanced nonsmall cell lung cancer. South Asian J Cancer 2017; 6: 143
- Jaiswal R, Pinninti R, Mohan MV, Santa A, Boyella PK, Nambaru L. et al. T790M mutation and clinical outcomes with osimertinib in patients with epidermal growth factor receptormutant nonsmall cell lung cancer. Indian J Med Paediatr Oncol 2019; 40: 73-8
- Zanwar S, Noronha V, Joshi A, Patil VM, Chougule A, Kumar R. et al. Repeat biopsy in epidermal growth factor receptor mutation-positive nonsmall cell lung cancer: Feasibility, limitations, and clinical utility in Indian patients. Indian J Cancer 2017; 54: 280-4
- Parikh PM, Bhattacharyya GS, Hingmire SS, Mehta P, Rangrajan B, Natrajan G. Our patient at risk from unauthorized, unapproved, illegally imported fake “generic medicines”. Indian J Med Sci 2018; 70: 43-7