Therapeutic strategies targeting the epidermal growth factor receptor signaling pathway in metastatic colorectal cancer

doi:10.4251/wjgo.v16.i6.2362

Advanced Search

BPG is committed to discovery and dissemination of knowledge

Home / Archive / Volume 16, Issue 6

This Article

Academic Content and Language Evaluation of This Article

CrossCheck and Google Search of This Article

Academic Rules and Norms of This Article

Citation of this article

Corresponding Author of This Article

Research Domain of This Article

Article-Type of This Article

Open-Access Policy of This Article

Times Cited Counts in Google of This Article

Number of Hits and Downloads for This Article

Total Article Views (227)

All Articles published online

The chart showing PDF series, HTML series, Figures (1-1) series, Tables (1-1) series.

Item

Count

PDF

HTML

140

Figures (1-1)

Tables (1-1)

Sum=202

Publishing Process of This Article

The chart showing Browse series, Download series.

Item

Count

Browse

Download

Sum=19

Jun 15, 2024 (publication date) through Jun 29, 2024

Times Cited of This Article

Times Cited (0)

Journal Information of This Article

Publication Name

World Journal of Gastrointestinal Oncology

ISSN

1948-5204

Publisher of This Article

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

Minireviews

World J Gastrointest Oncol. Jun 15, 2024; 16(6): 2362-2379
Published online Jun 15, 2024. doi: 10.4251/wjgo.v16.i6.2362

Table 1 Results of clinical trials based on RAS status

Therapy based on RAS status	Study	Design	Result	Ref.
RAS wild-type first-line therapy	CRYSTAL study	Cetuximab plus FOLFIRI vs FOLFIRI alone	The HR for PFS among patients with KRAS wild-type tumors was 0.68 (95%CI: 0.50 to 0.94), favoring the cetuximab-FOLFIRI group	Van Cutsem et al[4]
	OPUS study	Cetuximab plus FOLFOX-4 vs FOLFOX-4 alone	The median survival was 18.3 mo for patients receiving cetuximab plus FOLFOX-4 and 18.0 mo for FOLFOX-4 alone	Bokemeyer et al[5]
	COIN study	Cetuximab combined with the FOLFOX4 or XELOX regimen vs FOLFOX4 or XELOX regimen alone	The median survival was 19.6 mo vs 18.0 mo	Adams et al[6]
	PRIME study	Panitumumab combined with FOLFOX4 vs FOLFOX4 alone	In KRAS wild-type patients, panitumumab combined with FOLFOX4 significantly improved mPFS compared with FOLFOX4 alone, at 9.6 mo and 8.0 mo, respectively	Douillard et al[7]
RAS wild-type maintenance therapy	COIN-B study	Intermittent chemotherapy plus intermittent cetuximab therapy vs intermittent chemotherapy plus cetuximab maintenance therapy	mOS was 16.8 mo (95%CI: 14.5-22.6) in the intermittent cetuximab group vs 22.2 mo (18.4-28.9) in the continuous cetuximab group, and mPFS from week 12 was 3.1 mo (95%CI: 2.80-4.7) in the intermittent cetuximab group and 5.8 mo (4.9-8.6) with continuous cetuximab	Wasan et al[15]
	MACRO 2 TTD study	FOLFOX combined with cetuximab sequential cetuximab maintenance therapy vs FOLFOX combined with cetuximab	PFS at 9 mo was 60% vs 72%, and OS was 23 mo vs 27 mo. The objective response rate was 48% vs 39%	Aranda et al[16]
	MACBETH study	Modified FOLFOXIRI plus cetuximab, followed by cetuximab (arm A) vs bevacizumab maintenance (arm B)	10-mo PFR was 50.8% (90%CI: 39.5%-62.2%) in arm A and 40.4% (90%CI: 29.4%-52.1%) in arm B. The overall response rate was 71.6% (95%CI: 62.4%-79.5%)	Cremolini et al[17]
	VALENTINO study	Panitumumab plus fluorouracil and calcium folinate (arm A) vs panitumumab (arm B)	10-mo PFS rate was significantly higher in group A than in group B (59.9% vs 49.0%, P = 0.01). The mPFS was 12.0 mo and 9.9 mo, respectively. The OS rate at 18 mo was 66.4% and 62.4% (P = 0.60), respectively, with no significant difference	Pietrantonio et al[18]
	PANAMA (AIO KRK 0212) study	Panitumumab in combination with 5-FU vs 5-FU alone	RAS WT mCRC patients treated with 5-FU/LV + panitumumab maintenance therapy after FOLFOX + panitumumab induction therapy could have a superior outcome to 5-FU/LV maintenance therapy alone, with a PFS of 8.8 mo vs 5.7 mo (P = 0.014)	Modest et al[21]
RAS wild-type anti-EGFR-targeted agents rechallenge	CRICKET trial	Irinotecan and cetuximab as a third-line treatment for patients experiencing an initial response and then progression with a first-line irinotecan and cetuximab-containing therapy. Liquid biopsy samples were analyzed	The confirmed PR rate was 57% in patients with no RAS mutations detected in ctDNA. Patients with RAS wild-type ctDNA (n = 13) had significantly longer PFS than those with RAS-mutated ctDNA (n = 12), with a mPFS of 4.0 mo vs 1.9 mo (HR = 0.44, 95%CI: 0.18-0.98, P = 0.03), while no significant differences were reported in terms of OS (mOS: 12.5 mo vs 5.2 mo, HR = 0.58, 95%CI: 0.22-1.52, P = 0.24)	Cremolini et al[25]
	JACCRO CC-08 trial	Irinotecan plus cetuximab rechallenge as third-line treatment in KRAS wild-type mCRC patients who achieved clinical benefit with first-line cetuximab-containing therapy	The 3-mo PFS rate was 44.1%. The mPFS and OS were 2.4 mo and 8.2 mo, respectively. The response and DCR were 2.9% and 55.9%, respectively	Masuishi et al[26]
	CAPRI 2 GOIM trial	FOLFIRI + cetuximab (first line); FOLFOX + cetuximab (second line); irinotecan + cetuximab (third line)	Ongoing	Martini et al[28]
	WJOG8916G trial	TAS-102 in combination with cetuximab	DCR was 54%, PR was 3.6%, and mPFS was 2.4 mo. Patients with wild-type RAS, BRAF, EGFR, PIK3CA, ERBB2, and MET genes had a DCR of 75% vs 39% (P = 0.02), respectively, compared to mutant patients. mPFS was 4.7 mo vs 2.1 mo (P < 0.01)	Izawa et al[29]
	Phase II single-arm study	Cetuximab and palbociclib in KRAS-WT mCRC treated with ≥ 2 prior lines of therapy	The 4-mo DCR was 20%, which did not fulfill the prespecified 4-mo DCR rate. mPFS was 1.8 mo and mOS was 6.6 mo	Sorah et al[32]
	CAVE Trial	Cetuximab plus avelumab as a rechallenge strategy in patients with RAS wild-type metastatic colorectal cancer	The mOS was 17.3 mo for wild-type and 10.4 mo for ctDNA mutant patients (HR = 0.49, P = 0.02), with a PFS of 4.1 mo and 3.0 mo (HR = 0.42, P = 0.004), respectively	Martinelli et al[33]
	CAVE 2 study	Avelumab plus cetuximab as a reinvigorating strategy in pre-treated patients with RAS and BRAF WT mCRC	Ongoing	Napolitano et al[34]
	CRACK study	Cetuximab rechallenge combined with liposomal irinotecan and camrelizumab	The ORR was 25%, and the DCR was 75%. The mPFS and OS were 6.9 mo and 15.1 mo, respectively	Quan et al[36]
NeoRAS wild-type	C-PROWESS trial	Panitumumab plus irinotecan therapy for patients with NeoRAS mCRC	Ongoing	Osumi et al[40]
KRAS G12C mutation	CodeBreaK100 trial	Sotorasib	The ORR was 9.7%	Fakih et al[44]
	CodeBreaK300 trial	Sotorasib (960 mg daily in arm A and 240 mg daily in arm B) with panitumumab vs chemotherapy	HR = 0.49 (95%CI: 0.30-0.80, P = 0.006) in the sotorasib 960 + panitumumab group and HR = 0.58 (95%CI: 0.36-0.93, P = 0.03) in the sotorasib 240 + panitumumab group, and OS data was immature	Pietrantonio et al[45]
	KRYSTAL-1 study	Adagrasib (MRTX849) alone vs adagrasib plus cetuximab	In the adagrasib monotherapy group, the ORR and DCR were 19% and 86%, respectively, while the mPFS was 5.6 mo. In the cetuximab–adagrasib group, a higher ORR of 46% and DCR of 100% were observed, and the mPFS was 6.9 mo	Yaeger et al[46]

ORR: Overall response rate; mPFS: Median progression-free survival; OS: Overall survival; DCR: Disease control rate; HR: Hazard ratio; PFS: Progression-free survival; RAS: Rat sarcoma; KRAS: Kirsten RAS; ctDNA: Circulating tumor DNA; mCRC: Metastatic colorectal cancer; BRAF: B-type RAF.

Citation: Zhou Y, Wu S, Qu FJ. Therapeutic strategies targeting the epidermal growth factor receptor signaling pathway in metastatic colorectal cancer. World J Gastrointest Oncol 2024; 16(6): 2362-2379
URL: https://www.wjgnet.com/1948-5204/full/v16/i6/2362.htm
DOI: https://dx.doi.org/10.4251/wjgo.v16.i6.2362