Multimodal imaging and detection approach to ¹⁸F-FDG-directed surgery for patients with known or suspected malignancies: a comprehensive description of the specific methodology utilized in a single-institution cumulative retrospective experience

¹⁸F-fluorodeoxyglucose (¹⁸F-FDG) positron emission tomography/computed tomography (PET/CT) is widely used in the clinical management of cancer patients and has become the cornerstone of diagnostic imaging, staging, follow-up surveillance, and monitoring of ongoing therapy for a wide variety of malignancies [1‐7]. In this regard, there has been increased interest and growth in clinical research directed towards the use of ¹⁸F-FDG for the intraoperative detection of known and occult malignant disease during cancer surgery [8‐48]. The application of ¹⁸F-FDG for intraoperative detection during cancer surgery was first described in 1999 for colorectal cancer [8]. Since that time, a significant portion of this ongoing work related to the use of ¹⁸F-FDG for intraoperative detection during cancer surgery has been conducted at The Ohio State University and has been directed toward multiple solid malignancies [8‐10, 22‐24, 28‐33, 36, 37, 40]. Collectively, such efforts have been directed toward colorectal cancer, melanoma, lymphoma, breast cancer, gynecologic malignancies, head and neck malignancies, and lung cancer [8‐48]. The motivation behind using ¹⁸F-FDG for intraoperative detection during cancer surgery has been multifactorial, including exploring its applicability for real-time intraoperative staging, surgical planning and execution, and determination of completeness of surgical resection for ¹⁸F-FDG-avid lesions.

In 2007, we first reported upon our ongoing efforts to formulate a truly multimodal imaging and detection approach to ¹⁸F-FDG-directed surgery [23, 32, 36, 40]. In the general schema for this multimodal approach, patients undergoing same-day intravenous administration of ¹⁸F-FDG were subjected to one or more of a variety of ¹⁸F-FDG-related diagnostic procedures, including (1) same-day preoperative patient diagnostic PET/CT imaging, (2) intraoperative gamma probe assessment, (3) clinical PET/CT specimen scanning of whole surgically resected specimens (WSRS), research designated tissues (RDT), and/or sectioned research designated tissues (SRDT) (Table 1), (4) micro PET/CT specimen scanning of WSRS, RDT, and/or SRDT, (5) total radioactivity counting of each SRDT piece by an automatic gamma well counter, and (6) same-day postoperative patient diagnostic PET/CT imaging. Herein, we have comprehensively described the specific methodology utilized in our single-institution cumulative retrospective experience with a multimodal imaging and detection approach to ¹⁸F-FDG-directed surgery for patients with known or suspected malignancies, in order to assess its technical and logistic feasibility for real-time intraoperative staging, surgical planning and execution, and determination of completeness of surgical resection for ¹⁸F-FDG-avid lesions detected in patients who are deemed as appropriate surgical candidates.

A total of 145 patients were intravenously injected with ¹⁸F-FDG in anticipation for proceeding to the operating room on that same day for surgical exploration, biopsy, and possible resection of a known or suspected malignancy. This consisted of 98 females and 47 males. There were 134 Caucasian, eight African-American, and three Asian patients. Mean patient age was 57 (± 12, range 21-83) years. For all 145 participating patients, mean same-day ¹⁸F-FDG injection dose was 15.1 (± 3.5, range 4.6-26.1) mCi.

Of those 145 patients, a preoperative patient diagnostic PET/CT scan was done prior to the date of their anticipated ¹⁸F-FDG-directed surgery in 90 patients. In the remaining 55 patients, a preoperative patient diagnostic PET/CT scan was done on the same day as the anticipated ¹⁸F-FDG-directed surgery. For those 90 patients having their preoperative patient diagnostic PET/CT scan done prior to the day of their anticipated ¹⁸F-FDG-directed surgery, mean ¹⁸F-FDG injection dose for their prior preoperative patient diagnostic PET/CT scan was 14.3 (± 1.5, range 8.4-16.5) mCi, time from ¹⁸F-FDG injection to the preoperative patient diagnostic PET/CT scan was 80.6 (± 18, range 43-179) minutes, and mean duration of time from preoperative patient diagnostic PET/CT scan to the date of the anticipated ¹⁸F-FDG-directed surgery was 24 (± 18, range 1-92) days. For those 55 patients undergoing a same-day preoperative patient diagnostic PET/CT scan, mean same-day ¹⁸F-FDG injection dose was 16.4 (± 2.4, range 11.7-21.8) mCi and mean time from same-day ¹⁸F-FDG injection to their same-day preoperative patient diagnostic PET/CT scan was 73 (± 9, range 53-114) minutes.

Among the 145 patients intravenously injected with ¹⁸F-FDG in anticipation for proceeding to the operating room on that same day for surgical exploration, biopsy, and possible resection of a known or suspected malignancy, 142 were eventually taken to surgery on that same day. However, three of the same-day preoperative patient diagnostic PET/CT scans led to the cancellation of the anticipated surgical procedure. In two of these cases, same-day preoperative patient PET/CT scan demonstrated inoperable, widespread metastatic disease. In the other case, there was interval complete resolution of ¹⁸F-FDG avidity seen at the time of same-day preoperative patient diagnostic PET/CT scan as compared ¹⁸F-FDG avidity seen on a previously performed patient PET/CT scan.

Intraoperative gamma probe assessment was performed on 141 patients taken to the operating room for ¹⁸F-FDG-directed surgery. In the one case in which intraoperative gamma probe assessment was not performed, upon initial surgical exploration, it was noted that diffuse carcinomatosis was present, and resultantly, further surgical intervention was aborted. Mean time from same-day ¹⁸F-FDG injection to intraoperative gamma probe assessment was 286 (± 93, range 176-532) minutes.

WSRS were imaged by clinical PET/CT specimen scanning and micro PET/CT specimen scanning scan in 109 cases and 32 cases, respectively. Mean time from same-day ¹⁸F-FDG injection to scanning of WSRS by clinical PET/CT specimen scanning and micro PET/CT specimen scanning was 389 (± 148, range 86-741) minutes and 458 (± 97, range 272-656) minutes, respectively.

RDT were imaged by clinical PET/CT specimen scanning and micro PET/CT specimen scanning in 33 cases and 22 cases, respectively. Mean time from same-day ¹⁸F-FDG injection to scanning of RDT by clinical PET/CT specimen scanning and micro PET/CT specimen scanning was 619 (± 119, range 253-846) minutes and 661 (± 117, range 433-835) minutes, respectively.

SRDT pieces were imaged by clinical PET/CT specimen scanning and micro PET/CT specimen scanning in 49 cases and 26 cases, respectively. Mean time from same-day ¹⁸F-FDG injection to scanning of SRDT pieces by clinical PET/CT specimen scanning and micro PET/CT specimen scanning was 674 (± 186, range 299-1068) minutes and 752 (± 127, range 499-976) minutes, respectively. Tissue counting of individual SRDT pieces was performed on an automatic gamma well counter in 45 cases. Mean time from same-day ¹⁸F-FDG injection to performance of tissue counting of the SRDT pieces was 761 (± 187, range 324-1114) minutes.

A same-day postoperative patient diagnostic PET/CT scan was performed in 62 cases. Mean time from same-day ¹⁸F-FDG injection to the same-day postoperative patient diagnostic PET/CT scan was 516 (± 134, range 178-853) minutes.

Among the 142 patients who were taken to the operating room for ¹⁸F-FDG-directed surgery, 120 patients were found to have histologic confirmation of malignancy within their surgically resected specimens, 21 patients were found to have only benign pathology within their surgically resected specimens that were associated with their ¹⁸F-FDG-avid lesion(s) which were originally seen on their preoperative patient PET/CT scan, and one patient was intraoperatively found to have no detectable 18F-FDG-avid lesion (as well as no signs of disease on intraoperative ultrasound or on intraoperative visual inspection and palpation). Fourteen different histologic tumor types were represented within surgically resected specimens removed at the time of ¹⁸F-FDG-directed surgery from among the 120 patients with histologic confirmation of malignancy (Table 2). The three most common histologic tumor types found within surgically resected specimens were colorectal carcinoma (n = 66, 55.0%), breast carcinoma (n = 12, 10.0%), and lymphoma (n = 11, 9.2%). The region of localization of these 14 histologic tumor types among the 120 patients with histologic confirmation of malignancy was the abdomen and/or pelvis region in 87 cases (72.5%), the head and neck region in 12 cases (10.0%), the extremity, axillary, or inguinal regions in 12 cases (10.0%), and the chest region in 9 cases (7.5%).

The aim of this paper was to comprehensively describe the specific methodology utilized in our single-institution cumulative retrospective experience with a multimodal imaging and detection approach to ¹⁸F-FDG-directed surgery for patients with known or suspected malignancies. It is our belief that the information presented herein indicates that our multimodal imaging and detection approach to ¹⁸F-FDG-directed surgery for patients with known or suspected malignancies, utilizing a same-day ¹⁸F-FDG injection dose, is feasible from both a technical and a logistical perspective. This is evident from our ability to accomplish this coordination of services by the surgeon, radiologist, and pathologist in a same-day fashion. Such an integrated approach has the potential for allowing for: (1) real-time intraoperative staging of the extent of disease, (2) real-time intraoperative surgical planning and execution of the necessary and most appropriate operation, determination of the extent of surgical resection, and determination of the completeness of surgical resection, (3) real-time pathologic evaluation of intact surgical resected specimens for the confirmation of completeness of surgical resection and for surgical margin assessment, and (4) real-time pathologic evaluation of diagnostically biopsied tissues for confirmation of correctness of tissue diagnosis [32]. Since this paper purely represents a comprehensive description of the specific methodology utilized in our single-institution cumulative retrospective experience with a multimodal imaging and detection approach to ¹⁸F-FDG-directed surgery, and since this paper does not detail the specific cumulative results amassed from these 145 individual cases, it is the future plan of our current authorship to subsequently and systemically report upon many different aspects of our results, including analysis of image quality and sustainability of image quality seen on same-day preoperative patient diagnostic PET/CT imaging as it compares to same-day postoperative patient diagnostic PET/CT imaging, clinical PET/CT specimen imaging, micro PET/CT specimen imaging, automatic gamma well counter specimen activity, and intraoperative gamma probe assessment, as well as to report upon future clinical relevance, future clinical applications, and methodological limitations of this multimodal imaging and detection approach to ¹⁸F-FDG-directed surgery.

Whenever high-energy gamma photon emitting radiopharmaceuticals, such as ¹⁸F-FDG, are considered for routine use in the operating room environment, it is of importance to address the issue of radiation safety. In this specific regard, we have previously evaluated the occupational radiation exposure incurred by intraoperative and perioperative personnel involved during ¹⁸F-FDG-directed surgery cases [33]. In a comprehensive evaluation of 10 actual ¹⁸F-FDG-directed surgery cases, in which a mean dose of 18.9 mCi of ¹⁸F-FDG was intravenously injected at a mean time of 142 minutes prior to surgery, the resultant mean deep dose equivalent per case for the surgeon, anesthetist, scrub technologist, postoperative nurse, circulating nurse, and preoperative nurse was 164, 119, 92, 63, 54, and 48 μSv, respectively. Based upon the established annual occupational exposure limit for adults within the United States of a total effective dose equivalent of 50,000 μSv, as defined by the United States Nuclear Regulatory Commission [51], the estimated number of ¹⁸F-FDG-directed surgery cases per year and the estimated number of hours of exposure per year that could be theoretically incurred by the surgeon, anesthetist, scrub technologist, postoperative nurse, circulating nurse, and preoperative nurse were 305 cases and 820 hours, 420 cases and 1020 hours, 543 cases and 2083 hours, 794 cases and 1471 hours, 926 cases and 2941 hours, and 1042 cases and 602 hours, respectively. This data clearly illustrates that the absorbed radiation dose received by both intraoperative and perioperative personnel involved in ¹⁸F-FDG-directed surgery cases is relatively low per case and allows for all such personnel to participate in multiple cases and still remain well below regulatory standards set for occupational radiation exposure limits.

In summary, our multimodal imaging and detection approach to ¹⁸F-FDG-directed surgery for patients with known or suspected solid malignancies is technically and logistically feasible. It can be accomplished with coordination of services provided by the surgeon, radiologist, and pathologist in a same-day fashion. This integrated approach has the potential for allowing for real-time intraoperative staging, surgical planning and execution, and determination of the completion of surgical resection.