Positron emission tomography using [18F]fluorotamoxifen to evaluate therapeutic responses in patients with breast cancer: Preliminary study

Tomio Inoue; E. Edmund Kim; Sidney Wallace; David J. Yang; Franklin C.L. Wong; Pedro Bassa; Abdallah Cherif; Ebrahim Delpassand; Aman Buzdar; Donald A. Podoloff

doi:10.1089/cbr.1996.11.235

Positron emission tomography using [¹⁸F]fluorotamoxifen to evaluate therapeutic responses in patients with breast cancer: Preliminary study

Tomio Inoue, E. Edmund Kim, Sidney Wallace, David J. Yang, Franklin C.L. Wong, Pedro Bassa, Abdallah Cherif, Ebrahim Delpassand, Aman Buzdar, Donald A. Podoloff

Research output: Contribution to journal › Article › peer-review

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Abstract

Positron emission tomography (PET) was used to assess the biodistribution and clinical usefulness of [¹⁸F]fluorotamoxifen (FTX) in 10 patients with estrogen-receptor(ER)-positive breast tumors. Ten patients with ER-positive breast cancer were prospectively studied, and the consecutive PET imagings (each takes 15 or 20 min) were obtained for 60 or 80 rain after the injection of 88.8-392. 2 MBq (2. 4-10.6 mCi of [¹⁸F]FTX. Twenty three suspected primary or metastatic lesions in 10 patients were evaluated and the tumor uptakes of [¹⁸F]FTX in nineteen tumor lesions were correlated to the response of tamoxifen therapy. Three lesions in three patients were considered to be truly negative for breast cancer on the bases of biopsy specimens and/or clinical course. Five (71.4%) of seven patients and 16 (80.0%) of 20 lesions were interpreted to be truly positive for breast cancer. The mean standardized uptake value (SUV) of the radiotracer in tumor was 3.0 on delayed images. There was no significant correlation between the standardized uptake values of [¹⁸F]FTX and the ER concentrations in primary lesions. Nineteen tumor lesions in six patients were evaluable to compare the [¹⁸F]FTX uptake with responses to tamoxifen therapy after the PET study. Three patients who had a good response to tamoxifen therapy showed positive lesions on PET images, whereas two of three patients who had a poor response showed negative lesions and one showed mixed results. There was no significant difference of [¹⁸F]FTX uptake in bone lesions between good and poor responders. However, when bone lesions were excluded, [¹⁸F]FTX uptakes in tumors with good responses were significantly higher than those with poor responses (mean and standard deviation of SUV: 2.46 ± O.62 vs 1.37 ± 0.59, P< O.05) PET imaging using [¹⁸F]FTX provides useful information in predicting the effect of tamoxifen therapy in patients with ER-positive breast cancer. Further study is warranted to confirm the clinical utility of PET using [¹⁸F]FTX in breast cancer patients.

Original language	English (US)
Pages (from-to)	235-245
Number of pages	11
Journal	Cancer Biotherapy and Radiopharmaceuticals
Volume	11
Issue number	4
DOIs	https://doi.org/10.1089/cbr.1996.11.235
State	Published - Aug 1996

ASJC Scopus subject areas

Oncology
Radiology Nuclear Medicine and imaging
Pharmacology
Cancer Research

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Inoue, T., Kim, E. E., Wallace, S., Yang, D. J., Wong, F. C. L., Bassa, P., Cherif, A., Delpassand, E., Buzdar, A., & Podoloff, D. A. (1996). Positron emission tomography using [¹⁸F]fluorotamoxifen to evaluate therapeutic responses in patients with breast cancer: Preliminary study. Cancer Biotherapy and Radiopharmaceuticals, 11(4), 235-245. https://doi.org/10.1089/cbr.1996.11.235

Inoue, T, Kim, EE, Wallace, S, Yang, DJ, Wong, FCL, Bassa, P, Cherif, A, Delpassand, E, Buzdar, A & Podoloff, DA 1996, 'Positron emission tomography using [¹⁸F]fluorotamoxifen to evaluate therapeutic responses in patients with breast cancer: Preliminary study', Cancer Biotherapy and Radiopharmaceuticals, vol. 11, no. 4, pp. 235-245. https://doi.org/10.1089/cbr.1996.11.235

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title = "Positron emission tomography using [18F]fluorotamoxifen to evaluate therapeutic responses in patients with breast cancer: Preliminary study",

abstract = "Positron emission tomography (PET) was used to assess the biodistribution and clinical usefulness of [18F]fluorotamoxifen (FTX) in 10 patients with estrogen-receptor(ER)-positive breast tumors. Ten patients with ER-positive breast cancer were prospectively studied, and the consecutive PET imagings (each takes 15 or 20 min) were obtained for 60 or 80 rain after the injection of 88.8-392. 2 MBq (2. 4-10.6 mCi of [18F]FTX. Twenty three suspected primary or metastatic lesions in 10 patients were evaluated and the tumor uptakes of [18F]FTX in nineteen tumor lesions were correlated to the response of tamoxifen therapy. Three lesions in three patients were considered to be truly negative for breast cancer on the bases of biopsy specimens and/or clinical course. Five (71.4%) of seven patients and 16 (80.0%) of 20 lesions were interpreted to be truly positive for breast cancer. The mean standardized uptake value (SUV) of the radiotracer in tumor was 3.0 on delayed images. There was no significant correlation between the standardized uptake values of [18F]FTX and the ER concentrations in primary lesions. Nineteen tumor lesions in six patients were evaluable to compare the [18F]FTX uptake with responses to tamoxifen therapy after the PET study. Three patients who had a good response to tamoxifen therapy showed positive lesions on PET images, whereas two of three patients who had a poor response showed negative lesions and one showed mixed results. There was no significant difference of [18F]FTX uptake in bone lesions between good and poor responders. However, when bone lesions were excluded, [18F]FTX uptakes in tumors with good responses were significantly higher than those with poor responses (mean and standard deviation of SUV: 2.46 ± O.62 vs 1.37 ± 0.59, P< O.05) PET imaging using [18F]FTX provides useful information in predicting the effect of tamoxifen therapy in patients with ER-positive breast cancer. Further study is warranted to confirm the clinical utility of PET using [18F]FTX in breast cancer patients.",

author = "Tomio Inoue and Kim, {E. Edmund} and Sidney Wallace and Yang, {David J.} and Wong, {Franklin C.L.} and Pedro Bassa and Abdallah Cherif and Ebrahim Delpassand and Aman Buzdar and Podoloff, {Donald A.}",

year = "1996",

month = aug,

doi = "10.1089/cbr.1996.11.235",

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T2 - Preliminary study

AU - Inoue, Tomio

AU - Kim, E. Edmund

AU - Wallace, Sidney

AU - Yang, David J.

AU - Wong, Franklin C.L.

AU - Bassa, Pedro

AU - Cherif, Abdallah

AU - Delpassand, Ebrahim

AU - Buzdar, Aman

AU - Podoloff, Donald A.

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N2 - Positron emission tomography (PET) was used to assess the biodistribution and clinical usefulness of [18F]fluorotamoxifen (FTX) in 10 patients with estrogen-receptor(ER)-positive breast tumors. Ten patients with ER-positive breast cancer were prospectively studied, and the consecutive PET imagings (each takes 15 or 20 min) were obtained for 60 or 80 rain after the injection of 88.8-392. 2 MBq (2. 4-10.6 mCi of [18F]FTX. Twenty three suspected primary or metastatic lesions in 10 patients were evaluated and the tumor uptakes of [18F]FTX in nineteen tumor lesions were correlated to the response of tamoxifen therapy. Three lesions in three patients were considered to be truly negative for breast cancer on the bases of biopsy specimens and/or clinical course. Five (71.4%) of seven patients and 16 (80.0%) of 20 lesions were interpreted to be truly positive for breast cancer. The mean standardized uptake value (SUV) of the radiotracer in tumor was 3.0 on delayed images. There was no significant correlation between the standardized uptake values of [18F]FTX and the ER concentrations in primary lesions. Nineteen tumor lesions in six patients were evaluable to compare the [18F]FTX uptake with responses to tamoxifen therapy after the PET study. Three patients who had a good response to tamoxifen therapy showed positive lesions on PET images, whereas two of three patients who had a poor response showed negative lesions and one showed mixed results. There was no significant difference of [18F]FTX uptake in bone lesions between good and poor responders. However, when bone lesions were excluded, [18F]FTX uptakes in tumors with good responses were significantly higher than those with poor responses (mean and standard deviation of SUV: 2.46 ± O.62 vs 1.37 ± 0.59, P< O.05) PET imaging using [18F]FTX provides useful information in predicting the effect of tamoxifen therapy in patients with ER-positive breast cancer. Further study is warranted to confirm the clinical utility of PET using [18F]FTX in breast cancer patients.

AB - Positron emission tomography (PET) was used to assess the biodistribution and clinical usefulness of [18F]fluorotamoxifen (FTX) in 10 patients with estrogen-receptor(ER)-positive breast tumors. Ten patients with ER-positive breast cancer were prospectively studied, and the consecutive PET imagings (each takes 15 or 20 min) were obtained for 60 or 80 rain after the injection of 88.8-392. 2 MBq (2. 4-10.6 mCi of [18F]FTX. Twenty three suspected primary or metastatic lesions in 10 patients were evaluated and the tumor uptakes of [18F]FTX in nineteen tumor lesions were correlated to the response of tamoxifen therapy. Three lesions in three patients were considered to be truly negative for breast cancer on the bases of biopsy specimens and/or clinical course. Five (71.4%) of seven patients and 16 (80.0%) of 20 lesions were interpreted to be truly positive for breast cancer. The mean standardized uptake value (SUV) of the radiotracer in tumor was 3.0 on delayed images. There was no significant correlation between the standardized uptake values of [18F]FTX and the ER concentrations in primary lesions. Nineteen tumor lesions in six patients were evaluable to compare the [18F]FTX uptake with responses to tamoxifen therapy after the PET study. Three patients who had a good response to tamoxifen therapy showed positive lesions on PET images, whereas two of three patients who had a poor response showed negative lesions and one showed mixed results. There was no significant difference of [18F]FTX uptake in bone lesions between good and poor responders. However, when bone lesions were excluded, [18F]FTX uptakes in tumors with good responses were significantly higher than those with poor responses (mean and standard deviation of SUV: 2.46 ± O.62 vs 1.37 ± 0.59, P< O.05) PET imaging using [18F]FTX provides useful information in predicting the effect of tamoxifen therapy in patients with ER-positive breast cancer. Further study is warranted to confirm the clinical utility of PET using [18F]FTX in breast cancer patients.

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Positron emission tomography using [¹⁸F]fluorotamoxifen to evaluate therapeutic responses in patients with breast cancer: Preliminary study

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