Epidermal growth factor receptor and metastatic colorectal cancer: Insights into target therapies

doi:10.3748/wjg.v19.i38.6315

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Oct 14, 2013 (publication date) through Jul 22, 2024

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World Journal of Gastroenterology

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1007-9327

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Baishideng Publishing Group Inc, 7041 Koll Center Parkway, Suite 160, Pleasanton, CA 94566, USA

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World J Gastroenterol. Oct 14, 2013; 19(38): 6315-6318
Published online Oct 14, 2013. doi: 10.3748/wjg.v19.i38.6315

Table 1 Mainly clinical trial and target therapies

Study	Design	Median PFS (mo)	Median OS (mo)	Toxicity (grade 3/4)	Genetic analyses	Response rate
PACCE trial[18]	PMAB + Bev/Ox-CT	10	19.4	Skin rash, diarrhea, infections and pulmonary embolism	KRAS status was determined in 82% tumor samples. Mutations were found in 40%	46%
	+
	PMAB + Bev/Iri-CT
	Bev/Ox-CT	11.4	24.5			48%
	+
	Bev/Iri-CT
Peeters et al[22]	Panitumumab-FOLFIRI (in the WT KRAS subpopulation)	5.9	14.5¹	Toxicities associated with anti-EGFR therapy	KRAS status was available for 91% of patients: 597 (55%) with wild-type KRAS tumors, and 486 (45%) with mutant KRAS tumors	Improved to 35% vs 10% with the addition of panitumumab
Peeters et al[22]	FOLFIRI (in the WT KRAS subpopulation)	3.9	12.5¹	Toxicities associated with anti-EGFR therapy		Improved to 35% vs 10% with the addition of panitumumab
PRIME study[28]	Wild-type KRAS stratum Panitumumab +	9.6	23.9¹	Toxicities associated with anti-EGFR therapy	KRAS results were available for 1100 ( 93%)patients	55%
	FOLFOX (4)		23.9¹			55%
	FOLFOX(4)	8.0	19.7¹
	Mutant KRAS stratum					48%
	Panitumumab +	7.3	15.5¹			40%
	FOLFOX (4)
	FOLFOX (4)	8.8	19.3¹			40%
COIN trial[29]	Ox and 5FU (arm A) in KRAS wild-type tumours	8.6¹	17.9¹	NA	565 (43%) had KRAS mutations	57%
COIN trial[29]	Ox and 5FU plus cetuximab (arm B) in KRAS wild-type tumours	8.6¹	17.0¹	Skin rash and gastrointestinal toxic effects		64%
NORDIC-VII[20]	Standard Nordic FLOX (arm A)	7.9¹	20.4¹	The regimens were well tolerated	KRAS and BRAF mutation analyses were obtained in 498 (88%) and 457 patients (81%) respectively	41%
	Cetuximab and FLOX (arm B)	8.3¹	19.7¹	The regimens were well tolerated		49%
	Cetuximab combined with intermittent FLOX (arm C)	7.3¹	20.3¹			47%

¹Without statistical significance. PFS: Progression-free survival; OS: Overall survival; PMAB: Panitumumab; Bev: Bevacizumab; Ox:CT: Oxaliplatin:based chemotherapy; Iri-CT: Irinotecan-based chemotherapy; 5FU: 5-fluorouracil; FOLFOX/FLOX: Fluorouracil, leucovorin and oxaliplatin; FOLFIRI: Fluorouracil, leucovorin and irinotecan; NA: Not applicable.

Citation: Mello RA, Marques AM, Araújo A. Epidermal growth factor receptor and metastatic colorectal cancer: Insights into target therapies. World J Gastroenterol 2013; 19(38): 6315-6318
URL: https://www.wjgnet.com/1007-9327/full/v19/i38/6315.htm
DOI: https://dx.doi.org/10.3748/wjg.v19.i38.6315