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Poster Display

151P - Relationship between depth of response and early tumor shrinkage with overall survival in advanced pancreatic cancer

Date

02 Dec 2023

Session

Poster Display

Presenters

EMIKA KUROKI

Citation

Annals of Oncology (2023) 34 (suppl_4): S1520-S1555. 10.1016/annonc/annonc1379

Authors

E. KUROKI1, K. Nio2, M. Shimokawa3, T. Otsuka4, J. Nakazawa5, T. Shibuki6, S. Arima7, K. Miwa8, F. Koga9, Y. Ueda10, Y. Kubotsu11, H. Shimokawa12, S. Takeshita13, K. Nishikawa14, A. Hosokawa15, H. Oda16, S. Arita17, T. Shirakawa18, T. Mizuta19, K. Mitsugi20

Author affiliations

  • 1 Department Of Medical Oncology, Kagoshima City Hospital, 890-8760 - Kagoshima/JP
  • 2 Department Of Medical Oncology, Hamanomachi Hospital, 810-0072 - Fukuoka/JP
  • 3 Department Of Biostatistics, Yamaguchi University Graduate School of Medicine, 755-0046 - Yamaguchi/JP
  • 4 Department Of Internal Medicine, Minato Medical Clinic, Fukuoka/JP
  • 5 Department Of Medical Oncology, Kagoshima City Hospital, Kagoshima/JP
  • 6 Department Of Hepatobiliary And Pancreatology, National Cancer Center Hospital East, 277-8577 - Chiba/JP
  • 7 Digestive And Lifestyle Diseases, Kagoshima University Graduate school of Medical and Dental Sciences, 890-8520 - Kagoshima/JP
  • 8 Multidisciplinary Treatment Cancer Center, Kurume University Hospital, 830-0011 - Kurume/JP
  • 9 Department Of Hepatobiliary And Pancreatology, Saga Medical Center Koseikan, 840-8571 - Saga/JP
  • 10 Department Of Hematology And Oncology, Japanese Red Cross Kumamoto Hospital, 861-8520 - Kumamoto/JP
  • 11 Department Of Internal Medicine, Karatsu Red Cross Hospital, Saga/JP
  • 12 Department Of Hematology Oncology, Japan Community Healthcare Organization Kyushu Hospital, 806-8501 - Fukuoka/JP
  • 13 Department Of Gastroenterology, Japanese Red Cross Nagasaki Genbaku Hospital, 852-8511 - Nagasaki/JP
  • 14 Department Of Medical Oncology And Hematology, Oita University Faculty of Medicine, 879-5593 - Oita/JP
  • 15 Department Of Clinical Oncology, University of Miyazaki Hospital, 889-1692 - Miyazaki/JP
  • 16 Division Of Integrative Medical Oncology, Saiseikai Kumamoto Hospital, 861-4193 - Kumamoto/JP
  • 17 Department Of Internal Medicine And Chemotherapy, Miyazaki Prefectural Miyazaki Hospital, 880-8510 - Miyazaki/JP
  • 18 Department Of Internal Medicine, Karatsu Higashi-matsuura Medical Association Center, 847-0041 - Saga/JP
  • 19 Department Of Internal Medicine, Fujikawa Hospital, 840-0831 - Saga/JP
  • 20 Department Of Medical Oncology, Sasebo Kyosai Hospital, 857-8575 - Nagasaki/JP

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Abstract 151P

Background

Depth of response (DpR) and early tumor shrinkage (ETS) are established predictors of overall survival (OS) in colorectal and gastric cancer; however, data for pancreatic cancer (PC) are limited.

Methods

This study was conducted as part of two multicenter retrospective studies (NAPOLEON and NAPOLEON-2) of patients (pts) with measurable advanced PC tumors. Cohort 1 included 292 pts treated with gemcitabine/nab-PTX (GnP, 184 pts) and FOLFIRINOX (FFX, 108 pts) as first-line chemotherapy, and Cohort 2 included 88 pts treated with nanoliposomal irinotecan, fluorouracil and folinic acid as second-line chemotherapy. DpR was defined as the maximum tumor shrinkage percentage on imaging compared with the pre-treatment level. Pts were divided by DpR into three groups: control (Group A), responder (Group B), and deep responder (Group C). ETS was defined as ≥20% reduction from the start of treatment to the second evaluation.

Results

In Cohort 1, DpR was −2.3 to +1550% in Group A, −28.6 to −2.5% in Group B, and −100.0 to −28.6% in Group C. The baseline C-reactive protein/albumin ratio differed significantly by group (p=0.04). The median OS (mOS) was significantly longer in Group C (17.2 months) and Group B (11.5 months) than in Group A (8.4 months), (hazard ratio [HR], 95% confidence interval [CI]: 0.30, 0.22–0.42, p<0.01; and 0.58, 0.43–0.79, p<0.01, respectively). The mOS was also significantly longer in the ETS group overall (HR 0.46, 95% CI 0.35–0.61, p<0.01) and in both the GnP and FFX subgroups. In Cohort 2, DpR was +18.4 to +128.6% in Group A, −2.9 to +17.9% in Group B, and −80.0 to −3.2% in Group C. The baseline prevalence of ascites differed significantly by group (p=0.04). The mOS was significantly longer in Group C (10.9 months) than in Group A (4.6 months; HR 0.33, 95% CI 0.17–0.65, p<0.01), but mOS in Group B (6.8 months) did not differ significantly from Group A (p=0.10).

Conclusions

This is the first report that DpR and ETS might be predictors of OS in pts with PC on standard chemotherapy.

Clinical trial identification

Editorial acknowledgement

Legal entity responsible for the study

The authors.

Funding

Has not received any funding.

Disclosure

All authors have declared no conflicts of interest.

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