Hier finden Sie die aktuellsten Publikationen aus dem Gebiet der Nuklearmedizin in Österreich. Zusätzlich sind die Publikationen aus den Teilbereichen der PET, SPECT sowie nuklearmedizinischen Therapien unserer Kollegen in Österreich gesondert hervorgehoben.
Rezente Publikationen in Österreich
Transplant and Nontransplant Salvage Therapy in Pediatric Relapsed or Refractory Hodgkin Lymphoma: The EuroNet-PHL-R1 Phase 3 Nonrandomized Clinical Trial
Daw S, Claviez A, Kurch L, Stoevesandt D, Attarbaschi A, Balwierz W, Beishuizen A, Cepelova M, Ceppi F, Fernandez-Teijeiro A, Fosså A, Georgi TW, Hjalgrim LL, Hraskova A, Leblanc T, Mascarin M, Pears J, Landman-Parker J, Prelog T, Klapper W, Ramsay A, Kluge R, Dieckmann K, Pelz T, Vordermark D, Körholz D, Hasenclever D and Mauz-Körholz C
Transplant and Nontransplant Salvage Therapy in Pediatric Relapsed or Refractory Hodgkin Lymphoma: The EuroNet-PHL-R1 Phase 3 Nonrandomized Clinical Trial
Daw S, Claviez A, Kurch L, Stoevesandt D, Attarbaschi A, Balwierz W, Beishuizen A, Cepelova M, Ceppi F, Fernandez-Teijeiro A, Fosså A, Georgi TW, Hjalgrim LL, Hraskova A, Leblanc T, Mascarin M, Pears J, Landman-Parker J, Prelog T, Klapper W, Ramsay A, Kluge R, Dieckmann K, Pelz T, Vordermark D, Körholz D, Hasenclever D and Mauz-Körholz C
The current standard-of-care salvage therapy in relapsed/refractory classic Hodgkin lymphoma (cHL) includes consolidation high-dose chemotherapy (HDCT)/autologous stem cell transplant (aSCT).
Joint EANM/EANO/RANO/SNMMI practice guideline/procedure standard for PET imaging of brain metastases: version 1.0
Verger A, Tolboom N, Cicone F, Chang SM, Furtner J, Galldiks N, Gempt J, Guedj E, Huang RY, Johnson DR, Law I, Le Rhun E, Short SC, Bent MJVD, Weehaeghe DV, Vogelbaum MA, Wen PY, Albert NL and Preusser M
Joint EANM/EANO/RANO/SNMMI practice guideline/procedure standard for PET imaging of brain metastases: version 1.0
Verger A, Tolboom N, Cicone F, Chang SM, Furtner J, Galldiks N, Gempt J, Guedj E, Huang RY, Johnson DR, Law I, Le Rhun E, Short SC, Bent MJVD, Weehaeghe DV, Vogelbaum MA, Wen PY, Albert NL and Preusser M
This joint practice guideline/procedure standard was collaboratively developed by the European Association of Nuclear Medicine (EANM), the Society of Nuclear Medicine and Molecular Imaging (SNMMI), the European Association of Neuro-Oncology (EANO), and the PET task force of the Response Assessment in Neurooncology Working Group (PET/RANO). Brain metastases are the most common malignant central nervous system (CNS) tumors. PET imaging with radiolabeled amino acids and to lesser extent [F]FDG has gained considerable importance in the assessment of brain metastases, especially for the differential diagnosis between recurrent metastases and treatment-related changes which remains a limitation using conventional MRI. The aim of this guideline is to assist nuclear medicine physicians in recommending, performing, interpreting and reporting the results of brain PET imaging in patients with brain metastases. This practice guideline will define procedure standards for the application of PET imaging in patients with brain metastases in routine practice and clinical trials and will help to harmonize data acquisition and interpretation across centers.
B-CLL with negative F-FDG PET/CT and intensive solitary lesion on PSMA PET/CT mimicking prostate cancer bone metastases
Jung T, Neureiter D, Schweighofer-Zwink G, Rendl G, Pirich C and Beheshti M
B-CLL with negative F-FDG PET/CT and intensive solitary lesion on PSMA PET/CT mimicking prostate cancer bone metastases
Jung T, Neureiter D, Schweighofer-Zwink G, Rendl G, Pirich C and Beheshti M
Positron emission tomography/computed tomography (PET/CT) using prostate-specific membrane antigen (PSMA)-radioligands is currently suggested by several clinical guidelines for the assessment of prostate cancer (PCa) in various clinical settings. However, PSMA will also be overexpressed in different cancers, which should be considered on the PSMA PET/CT reading in patients with concomitant neoplastic diseases. We report a case of 82-year-old male presented with prostate and history of oesophageal cancer and B-cell chronic lymphocytic leukemia (B-CLL). Both Ga-PSMA-11 and 2-(3-(1-carboxy-5-((6-(18f)fluoro-pyridine-3-carbonyl)-amino)-pentyl)-ureido)-pentanedioic acid (F-DCFPyL) PET/CT, which were performed for prostate cancer staging and re-staging in about 1 year interval, showed focal uptake in the primary prostate tumor as well as an intense focal lesion in L2, suggestive of bone metastasis. F-FDG PET/CT scans performed before and after PSMA PET/CT examinations showed no abnormal uptake related to oesophageal and/or B-CLL. This pattern could present an oligometastatic PCa disease, which might change the treatment plan of the patient to radiation of the bone metastasis. However, bone biopsy of the detected lesion on L2 revealed infiltrates of B-CLL. The role of Ga- and F-labeled PSMA PET/CT in prostate cancer is evolving and has been demonstrated to have high sensitivity, but may present limited specificity in patients with coexisting cancer(s), which should be considered in PSMA PET/CT reading.
Results of F-choline and C-methionine positron emission tomography/computed tomography for the preoperative localization of hyperfunctional parathyroid glands in primary hyperparathyroidism
Weber T, Smaxwil C, Hermann M, Lenschow C, Lorenz K, Steinmüller T, Trupka A, Negele T, Holzer K, Tzatzarakis E, Eilsberger F, Eberhardt N, Klinger C and Peth S
Results of F-choline and C-methionine positron emission tomography/computed tomography for the preoperative localization of hyperfunctional parathyroid glands in primary hyperparathyroidism
Weber T, Smaxwil C, Hermann M, Lenschow C, Lorenz K, Steinmüller T, Trupka A, Negele T, Holzer K, Tzatzarakis E, Eilsberger F, Eberhardt N, Klinger C and Peth S
Preoperative localization of hyperfunctioning parathyroid glands in primary hyperparathyroidism is essential for successful parathyroid surgery, particularly in patients with previous negative imaging or reoperations.
Preclinical evaluation of the potential PARP-imaging probe [carbonyl-C]DPQ
Benčurová K, Balber T, Weissenböck V, Kogler L, Friske J, Pichler V, Mitterhauser M, Hacker M, Philippe C and Ozenil M
Preclinical evaluation of the potential PARP-imaging probe [carbonyl-C]DPQ
Benčurová K, Balber T, Weissenböck V, Kogler L, Friske J, Pichler V, Mitterhauser M, Hacker M, Philippe C and Ozenil M
Poly (ADP-ribose) polymerase (PARP) enzymes are crucial for the repair of DNA single-strand breaks and have become key therapeutic targets in homologous recombination-deficient cancers, including prostate cancer. To enable non-invasive monitoring of PARP-1 expression, several PARP-1-targeting positron emission tomography (PET) tracers have been developed. Here, we aimed to preclinically investigate [carbonyl-C]DPQ as an alternative PARP-1 PET tracer as it features a strongly distinct chemotype compared to the frontrunners [F]FluorThanatrace and [F]PARPi.
Molecular Stratification of Light-Chain Cardiac Amyloidosis With F-Florbetapir and Ga-FAPI-04 for Enhanced Prognostic Precision
Wang X, Shen K, Zhang Y, Gao Y, Liu B, Guo Y, Ren C, Huang Z, Li X, Chang L, Ding H, Zhang H, Tian Z, Hacker M, Zhang S, Wang Y, Li J, Li X and Huo L
Molecular Stratification of Light-Chain Cardiac Amyloidosis With F-Florbetapir and Ga-FAPI-04 for Enhanced Prognostic Precision
Wang X, Shen K, Zhang Y, Gao Y, Liu B, Guo Y, Ren C, Huang Z, Li X, Chang L, Ding H, Zhang H, Tian Z, Hacker M, Zhang S, Wang Y, Li J, Li X and Huo L
Cardiac involvement in amyloid light chain (AL) amyloidosis significantly influences prognosis, necessitating timely diagnosis and meticulous risk stratification.
Safety, Biodistribution, and Radiation Dosimetry of the Ga-Labeled Minigastrin Analog DOTA-MGS5 in Patients with Advanced Medullary Thyroid Cancer and Other Neuroendocrine Tumors
von Guggenberg E, di Santo G, Uprimny C, Bayerschmidt S, Warwitz B, Hörmann AA, Zavvar TS, Rangger C, Decristoforo C, Sviridenko A, Nilica B, Santo G and Virgolini IJ
Safety, Biodistribution, and Radiation Dosimetry of the Ga-Labeled Minigastrin Analog DOTA-MGS5 in Patients with Advanced Medullary Thyroid Cancer and Other Neuroendocrine Tumors
von Guggenberg E, di Santo G, Uprimny C, Bayerschmidt S, Warwitz B, Hörmann AA, Zavvar TS, Rangger C, Decristoforo C, Sviridenko A, Nilica B, Santo G and Virgolini IJ
Several exploratory studies have demonstrated the feasibility of cholecystokinin-2 receptor (CCK2R) targeting in patients with medullary thyroid carcinoma (MTC) and other neuroendocrine tumors (NETs). We report the results of a prospective phase I/IIA pilot study (clinicaltrials.gov NCT06155994) conducted at our center with the Ga-labeled peptide analog DOTA-DGlu-Ala-Tyr-Gly-Trp-(N-Me)Nle-Asp-1-Nal-Phe-NH (Ga-DOTA-MGS5). Six patients with advanced MTC and 6 patients with gastroenteropancreatic and bronchopulmonary NETs confirmed by previous PET/CT imaging with other PET tracers received a single dose of 180 MBq of Ga-DOTA-MGS5. The first 6 patients enrolled in the study were included in the dosimetry evaluation, and safety was assessed in all 12 patients. PET/CT imaging was performed at different time points after injection to perform dosimetric calculations and to determine the optimal imaging time window. In addition, blood and urine samples were collected for pharmacokinetic assessments. The administration of Ga-DOTA-MGS5 was well tolerated, with minor adverse drug reactions occurring only in 3 patients. Ga-DOTA-MGS5 was cleared rapidly from the blood, with less than 21% of the injected activity present in blood 215 ± 10 min after injection. Tracer elimination occurred mainly through the kidneys, with a cumulative urinary excretion greater than 40% 3 h after injection. A high percentage of intact radiopeptide was confirmed in plasma. The highest absorbed dose was found for the urinary bladder wall, the stomach wall, and the kidneys, with an effective dose of 0.023 ± 0.007 mSv/MBq. The time points of 1 and 2 h after injection proved to be optimal for PET/CT imaging. In the 6 patients included in the dosimetry evaluation, local metastasis was confirmed in 2 patients with advanced MTC, whereas only 1 of 4 patients with gastroenteropancreatic NETs was positive in Ga-DOTA-MGS5 PET/CT. Besides confirming the safety of administration, within the phase I part of the prospective clinical trial, an acceptable effective whole-body dose, an overall favorable biodistribution, and the feasibility of cholecystokinin-2 receptor imaging could be shown for Ga-DOTA-MGS5.
Influence of dosimetry accuracy on the correlation with treatment outcome in a preliminary PSMA radiopharmaceutical therapy study
Hu J, Seifert R, Karkampouna S, Gomes CV, Xue S, Afshar-Ormieh A, Rominger A and Shi K
Influence of dosimetry accuracy on the correlation with treatment outcome in a preliminary PSMA radiopharmaceutical therapy study
Hu J, Seifert R, Karkampouna S, Gomes CV, Xue S, Afshar-Ormieh A, Rominger A and Shi K
Despite the potential of dosimetry in optimizing personalized radiopharmaceutical therapy (RPT), its limited clinical implementation impedes the development of simplified protocols for routine adoption. However, simplifications may introduce errors in dosimetry, prompting questions about their impact on clinical practice.
Comparison of Two Chelator Scaffolds as Basis for Cholecystokinin-2 Receptor Targeting Bimodal Imaging Probes
Gariglio G, Bendova K, Hermann M, Olafsdottir A, Sosabowski JK, Petrik M, von Guggenberg E and Decristoforo C
Comparison of Two Chelator Scaffolds as Basis for Cholecystokinin-2 Receptor Targeting Bimodal Imaging Probes
Gariglio G, Bendova K, Hermann M, Olafsdottir A, Sosabowski JK, Petrik M, von Guggenberg E and Decristoforo C
: Dual-modality probes, combining positron emission tomography (PET) with fluorescence imaging (FI) capabilities in a single molecule, are of high relevance for the accurate staging and guided resection of tumours. We herein present a pair of candidates targeting the cholecystokinin-2 receptor (CCK2R), namely [Ga]Ga-CyTMG and [Ga]Ga-CyFMG. In these probes, the SulfoCy5.5 fluorophore and two units of a CCK2R-binding motif are coupled to the chelator acting as a core scaffold, triazacyclononane-phosphinic acid (TRAP), and Fusarinine C (FSC), respectively. Using this approach, we investigated the influence of these chelators on the final properties. : The synthetic strategy to both precursors was based on the stoichiometric conjugation of the components via click chemistry. The characterization in vitro included the evaluation of the CCK2R affinity and internalization in A431-CCK2R cells. Ex vivo biodistribution as well as PET and FI studies were performed in xenografted mice. : Ga labelling was accomplished with high radiochemical yield and purity for both precursors. A CCK2R affinity in the subnanomolar range of the conjugates and a receptor-specific uptake of the radioligands in cells were observed. In A431-CCK2R/A431-mock xenografted mice, the investigated compounds showed specific accumulation in the tumours and reduced off-target uptake compared to a previously developed compound. Higher accumulation and prolonged retention in the kidneys were observed for [Ga]Ga-CyTMG when compared to [Ga]Ga-CyFMG. Despite the promising targeting properties observed, further probe optimization is required to achieve enhanced imaging contrast at early timepoints. Additionally, the results indicate a distinct influence of the chelators in terms of renal accumulation and retention.
Evaluation of early metabolic changes following vorasidenib using FET PET in patients with -mutant gliomas
Galldiks N, Werner JM, Stetter I, Puhr HC, Nakuz TS, Stoffels G, Albert NL, Langen KJ, Lohmann P and Preusser M
Evaluation of early metabolic changes following vorasidenib using FET PET in patients with -mutant gliomas
Galldiks N, Werner JM, Stetter I, Puhr HC, Nakuz TS, Stoffels G, Albert NL, Langen KJ, Lohmann P and Preusser M
The phase-3 INDIGO trial demonstrated that the isocitrate dehydrogenase () inhibitor vorasidenib significantly prolonged progression-free survival and delayed intervention in patients with CNS WHO grade 2 gliomas. However, conventional MRI showed limited response, with only 11% of patients having objective responses. Studies suggest that serial PET imaging with radiolabeled amino acids, such as -(2-[ F]-fluoroethyl)-L-tyrosine (FET) PET, may provide earlier and more informative assessments of treatment response than MRI. In an initial experience with FET PET, 3 out of 5 patients showed metabolic response to vorasidenib. This highlights FET PET's potential to guide decision-making, though further trials are needed to confirm outcome benefits.
Teilbereich PET
Transplant and Nontransplant Salvage Therapy in Pediatric Relapsed or Refractory Hodgkin Lymphoma: The EuroNet-PHL-R1 Phase 3 Nonrandomized Clinical Trial
Daw S, Claviez A, Kurch L, Stoevesandt D, Attarbaschi A, Balwierz W, Beishuizen A, Cepelova M, Ceppi F, Fernandez-Teijeiro A, Fosså A, Georgi TW, Hjalgrim LL, Hraskova A, Leblanc T, Mascarin M, Pears J, Landman-Parker J, Prelog T, Klapper W, Ramsay A, Kluge R, Dieckmann K, Pelz T, Vordermark D, Körholz D, Hasenclever D and Mauz-Körholz C
Transplant and Nontransplant Salvage Therapy in Pediatric Relapsed or Refractory Hodgkin Lymphoma: The EuroNet-PHL-R1 Phase 3 Nonrandomized Clinical Trial
Daw S, Claviez A, Kurch L, Stoevesandt D, Attarbaschi A, Balwierz W, Beishuizen A, Cepelova M, Ceppi F, Fernandez-Teijeiro A, Fosså A, Georgi TW, Hjalgrim LL, Hraskova A, Leblanc T, Mascarin M, Pears J, Landman-Parker J, Prelog T, Klapper W, Ramsay A, Kluge R, Dieckmann K, Pelz T, Vordermark D, Körholz D, Hasenclever D and Mauz-Körholz C
The current standard-of-care salvage therapy in relapsed/refractory classic Hodgkin lymphoma (cHL) includes consolidation high-dose chemotherapy (HDCT)/autologous stem cell transplant (aSCT).
Joint EANM/EANO/RANO/SNMMI practice guideline/procedure standard for PET imaging of brain metastases: version 1.0
Verger A, Tolboom N, Cicone F, Chang SM, Furtner J, Galldiks N, Gempt J, Guedj E, Huang RY, Johnson DR, Law I, Le Rhun E, Short SC, Bent MJVD, Weehaeghe DV, Vogelbaum MA, Wen PY, Albert NL and Preusser M
Joint EANM/EANO/RANO/SNMMI practice guideline/procedure standard for PET imaging of brain metastases: version 1.0
Verger A, Tolboom N, Cicone F, Chang SM, Furtner J, Galldiks N, Gempt J, Guedj E, Huang RY, Johnson DR, Law I, Le Rhun E, Short SC, Bent MJVD, Weehaeghe DV, Vogelbaum MA, Wen PY, Albert NL and Preusser M
This joint practice guideline/procedure standard was collaboratively developed by the European Association of Nuclear Medicine (EANM), the Society of Nuclear Medicine and Molecular Imaging (SNMMI), the European Association of Neuro-Oncology (EANO), and the PET task force of the Response Assessment in Neurooncology Working Group (PET/RANO). Brain metastases are the most common malignant central nervous system (CNS) tumors. PET imaging with radiolabeled amino acids and to lesser extent [F]FDG has gained considerable importance in the assessment of brain metastases, especially for the differential diagnosis between recurrent metastases and treatment-related changes which remains a limitation using conventional MRI. The aim of this guideline is to assist nuclear medicine physicians in recommending, performing, interpreting and reporting the results of brain PET imaging in patients with brain metastases. This practice guideline will define procedure standards for the application of PET imaging in patients with brain metastases in routine practice and clinical trials and will help to harmonize data acquisition and interpretation across centers.
B-CLL with negative F-FDG PET/CT and intensive solitary lesion on PSMA PET/CT mimicking prostate cancer bone metastases
Jung T, Neureiter D, Schweighofer-Zwink G, Rendl G, Pirich C and Beheshti M
B-CLL with negative F-FDG PET/CT and intensive solitary lesion on PSMA PET/CT mimicking prostate cancer bone metastases
Jung T, Neureiter D, Schweighofer-Zwink G, Rendl G, Pirich C and Beheshti M
Positron emission tomography/computed tomography (PET/CT) using prostate-specific membrane antigen (PSMA)-radioligands is currently suggested by several clinical guidelines for the assessment of prostate cancer (PCa) in various clinical settings. However, PSMA will also be overexpressed in different cancers, which should be considered on the PSMA PET/CT reading in patients with concomitant neoplastic diseases. We report a case of 82-year-old male presented with prostate and history of oesophageal cancer and B-cell chronic lymphocytic leukemia (B-CLL). Both Ga-PSMA-11 and 2-(3-(1-carboxy-5-((6-(18f)fluoro-pyridine-3-carbonyl)-amino)-pentyl)-ureido)-pentanedioic acid (F-DCFPyL) PET/CT, which were performed for prostate cancer staging and re-staging in about 1 year interval, showed focal uptake in the primary prostate tumor as well as an intense focal lesion in L2, suggestive of bone metastasis. F-FDG PET/CT scans performed before and after PSMA PET/CT examinations showed no abnormal uptake related to oesophageal and/or B-CLL. This pattern could present an oligometastatic PCa disease, which might change the treatment plan of the patient to radiation of the bone metastasis. However, bone biopsy of the detected lesion on L2 revealed infiltrates of B-CLL. The role of Ga- and F-labeled PSMA PET/CT in prostate cancer is evolving and has been demonstrated to have high sensitivity, but may present limited specificity in patients with coexisting cancer(s), which should be considered in PSMA PET/CT reading.
Results of F-choline and C-methionine positron emission tomography/computed tomography for the preoperative localization of hyperfunctional parathyroid glands in primary hyperparathyroidism
Weber T, Smaxwil C, Hermann M, Lenschow C, Lorenz K, Steinmüller T, Trupka A, Negele T, Holzer K, Tzatzarakis E, Eilsberger F, Eberhardt N, Klinger C and Peth S
Results of F-choline and C-methionine positron emission tomography/computed tomography for the preoperative localization of hyperfunctional parathyroid glands in primary hyperparathyroidism
Weber T, Smaxwil C, Hermann M, Lenschow C, Lorenz K, Steinmüller T, Trupka A, Negele T, Holzer K, Tzatzarakis E, Eilsberger F, Eberhardt N, Klinger C and Peth S
Preoperative localization of hyperfunctioning parathyroid glands in primary hyperparathyroidism is essential for successful parathyroid surgery, particularly in patients with previous negative imaging or reoperations.
Preclinical evaluation of the potential PARP-imaging probe [carbonyl-C]DPQ
Benčurová K, Balber T, Weissenböck V, Kogler L, Friske J, Pichler V, Mitterhauser M, Hacker M, Philippe C and Ozenil M
Preclinical evaluation of the potential PARP-imaging probe [carbonyl-C]DPQ
Benčurová K, Balber T, Weissenböck V, Kogler L, Friske J, Pichler V, Mitterhauser M, Hacker M, Philippe C and Ozenil M
Poly (ADP-ribose) polymerase (PARP) enzymes are crucial for the repair of DNA single-strand breaks and have become key therapeutic targets in homologous recombination-deficient cancers, including prostate cancer. To enable non-invasive monitoring of PARP-1 expression, several PARP-1-targeting positron emission tomography (PET) tracers have been developed. Here, we aimed to preclinically investigate [carbonyl-C]DPQ as an alternative PARP-1 PET tracer as it features a strongly distinct chemotype compared to the frontrunners [F]FluorThanatrace and [F]PARPi.
Molecular Stratification of Light-Chain Cardiac Amyloidosis With F-Florbetapir and Ga-FAPI-04 for Enhanced Prognostic Precision
Wang X, Shen K, Zhang Y, Gao Y, Liu B, Guo Y, Ren C, Huang Z, Li X, Chang L, Ding H, Zhang H, Tian Z, Hacker M, Zhang S, Wang Y, Li J, Li X and Huo L
Molecular Stratification of Light-Chain Cardiac Amyloidosis With F-Florbetapir and Ga-FAPI-04 for Enhanced Prognostic Precision
Wang X, Shen K, Zhang Y, Gao Y, Liu B, Guo Y, Ren C, Huang Z, Li X, Chang L, Ding H, Zhang H, Tian Z, Hacker M, Zhang S, Wang Y, Li J, Li X and Huo L
Cardiac involvement in amyloid light chain (AL) amyloidosis significantly influences prognosis, necessitating timely diagnosis and meticulous risk stratification.
Safety, Biodistribution, and Radiation Dosimetry of the Ga-Labeled Minigastrin Analog DOTA-MGS5 in Patients with Advanced Medullary Thyroid Cancer and Other Neuroendocrine Tumors
von Guggenberg E, di Santo G, Uprimny C, Bayerschmidt S, Warwitz B, Hörmann AA, Zavvar TS, Rangger C, Decristoforo C, Sviridenko A, Nilica B, Santo G and Virgolini IJ
Safety, Biodistribution, and Radiation Dosimetry of the Ga-Labeled Minigastrin Analog DOTA-MGS5 in Patients with Advanced Medullary Thyroid Cancer and Other Neuroendocrine Tumors
von Guggenberg E, di Santo G, Uprimny C, Bayerschmidt S, Warwitz B, Hörmann AA, Zavvar TS, Rangger C, Decristoforo C, Sviridenko A, Nilica B, Santo G and Virgolini IJ
Several exploratory studies have demonstrated the feasibility of cholecystokinin-2 receptor (CCK2R) targeting in patients with medullary thyroid carcinoma (MTC) and other neuroendocrine tumors (NETs). We report the results of a prospective phase I/IIA pilot study (clinicaltrials.gov NCT06155994) conducted at our center with the Ga-labeled peptide analog DOTA-DGlu-Ala-Tyr-Gly-Trp-(N-Me)Nle-Asp-1-Nal-Phe-NH (Ga-DOTA-MGS5). Six patients with advanced MTC and 6 patients with gastroenteropancreatic and bronchopulmonary NETs confirmed by previous PET/CT imaging with other PET tracers received a single dose of 180 MBq of Ga-DOTA-MGS5. The first 6 patients enrolled in the study were included in the dosimetry evaluation, and safety was assessed in all 12 patients. PET/CT imaging was performed at different time points after injection to perform dosimetric calculations and to determine the optimal imaging time window. In addition, blood and urine samples were collected for pharmacokinetic assessments. The administration of Ga-DOTA-MGS5 was well tolerated, with minor adverse drug reactions occurring only in 3 patients. Ga-DOTA-MGS5 was cleared rapidly from the blood, with less than 21% of the injected activity present in blood 215 ± 10 min after injection. Tracer elimination occurred mainly through the kidneys, with a cumulative urinary excretion greater than 40% 3 h after injection. A high percentage of intact radiopeptide was confirmed in plasma. The highest absorbed dose was found for the urinary bladder wall, the stomach wall, and the kidneys, with an effective dose of 0.023 ± 0.007 mSv/MBq. The time points of 1 and 2 h after injection proved to be optimal for PET/CT imaging. In the 6 patients included in the dosimetry evaluation, local metastasis was confirmed in 2 patients with advanced MTC, whereas only 1 of 4 patients with gastroenteropancreatic NETs was positive in Ga-DOTA-MGS5 PET/CT. Besides confirming the safety of administration, within the phase I part of the prospective clinical trial, an acceptable effective whole-body dose, an overall favorable biodistribution, and the feasibility of cholecystokinin-2 receptor imaging could be shown for Ga-DOTA-MGS5.
Effect of statins on arterial wall inflammation as assessed by 18F-FDG PET CT: an updated systematic review and meta-analysis
Jamialahmadi T, Reiner Ž, Simental-Mendia LE, Almahmeed W, Karav S, Eid AH, Giammarile F and Sahebkar A
Effect of statins on arterial wall inflammation as assessed by 18F-FDG PET CT: an updated systematic review and meta-analysis
Jamialahmadi T, Reiner Ž, Simental-Mendia LE, Almahmeed W, Karav S, Eid AH, Giammarile F and Sahebkar A
Pathogenesis of atherosclerosis is largely mediated by inflammatory process. Statins are lipid-lowering drugs which also have anti-inflammatory effects. 18 fluorine radiolabeled fluorodeoxyglucose (18 F-FDG) positron emission tomography-computed tomography (PET-CT) is considered to be a good indicator of arterial wall inflammation. Therefore, in this meta-analysis the role of statins on inflammatory process in the artery wall was evaluated using this method since its actual validity for this purpose is not yet well established.
Comparison of Two Chelator Scaffolds as Basis for Cholecystokinin-2 Receptor Targeting Bimodal Imaging Probes
Gariglio G, Bendova K, Hermann M, Olafsdottir A, Sosabowski JK, Petrik M, von Guggenberg E and Decristoforo C
Comparison of Two Chelator Scaffolds as Basis for Cholecystokinin-2 Receptor Targeting Bimodal Imaging Probes
Gariglio G, Bendova K, Hermann M, Olafsdottir A, Sosabowski JK, Petrik M, von Guggenberg E and Decristoforo C
: Dual-modality probes, combining positron emission tomography (PET) with fluorescence imaging (FI) capabilities in a single molecule, are of high relevance for the accurate staging and guided resection of tumours. We herein present a pair of candidates targeting the cholecystokinin-2 receptor (CCK2R), namely [Ga]Ga-CyTMG and [Ga]Ga-CyFMG. In these probes, the SulfoCy5.5 fluorophore and two units of a CCK2R-binding motif are coupled to the chelator acting as a core scaffold, triazacyclononane-phosphinic acid (TRAP), and Fusarinine C (FSC), respectively. Using this approach, we investigated the influence of these chelators on the final properties. : The synthetic strategy to both precursors was based on the stoichiometric conjugation of the components via click chemistry. The characterization in vitro included the evaluation of the CCK2R affinity and internalization in A431-CCK2R cells. Ex vivo biodistribution as well as PET and FI studies were performed in xenografted mice. : Ga labelling was accomplished with high radiochemical yield and purity for both precursors. A CCK2R affinity in the subnanomolar range of the conjugates and a receptor-specific uptake of the radioligands in cells were observed. In A431-CCK2R/A431-mock xenografted mice, the investigated compounds showed specific accumulation in the tumours and reduced off-target uptake compared to a previously developed compound. Higher accumulation and prolonged retention in the kidneys were observed for [Ga]Ga-CyTMG when compared to [Ga]Ga-CyFMG. Despite the promising targeting properties observed, further probe optimization is required to achieve enhanced imaging contrast at early timepoints. Additionally, the results indicate a distinct influence of the chelators in terms of renal accumulation and retention.
Evaluation of early metabolic changes following vorasidenib using FET PET in patients with -mutant gliomas
Galldiks N, Werner JM, Stetter I, Puhr HC, Nakuz TS, Stoffels G, Albert NL, Langen KJ, Lohmann P and Preusser M
Evaluation of early metabolic changes following vorasidenib using FET PET in patients with -mutant gliomas
Galldiks N, Werner JM, Stetter I, Puhr HC, Nakuz TS, Stoffels G, Albert NL, Langen KJ, Lohmann P and Preusser M
The phase-3 INDIGO trial demonstrated that the isocitrate dehydrogenase () inhibitor vorasidenib significantly prolonged progression-free survival and delayed intervention in patients with CNS WHO grade 2 gliomas. However, conventional MRI showed limited response, with only 11% of patients having objective responses. Studies suggest that serial PET imaging with radiolabeled amino acids, such as -(2-[ F]-fluoroethyl)-L-tyrosine (FET) PET, may provide earlier and more informative assessments of treatment response than MRI. In an initial experience with FET PET, 3 out of 5 patients showed metabolic response to vorasidenib. This highlights FET PET's potential to guide decision-making, though further trials are needed to confirm outcome benefits.
Teilbereich SPECT
Prognostic implication of DPD quantification in transthyretin cardiac amyloidosis
Rettl R, Duca F, Kronberger C, Binder C, Willixhofer R, Ermolaev N, Poledniczek M, Hofer F, Nitsche C, Hengstenberg C, Eslam RB, Kastner J, Bergler-Klein J, Hacker M, Calabretta R and Kammerlander AA
Prognostic implication of DPD quantification in transthyretin cardiac amyloidosis
Rettl R, Duca F, Kronberger C, Binder C, Willixhofer R, Ermolaev N, Poledniczek M, Hofer F, Nitsche C, Hengstenberg C, Eslam RB, Kastner J, Bergler-Klein J, Hacker M, Calabretta R and Kammerlander AA
Quantification of cardiac [99mTc]-3,3-diphosphono-1,2-propanodicarboxylic acid (DPD) uptake enhances diagnostic capabilities and may facilitate prognostic stratification in patients with transthyretin cardiac amyloidosis (ATTR-CA). This study aimed to evaluate the association of quantitative left ventricular (LV) DPD uptake with myocardial structure and function, and their implications on outcome in ATTR-CA.
Dopaminergic PET to SPECT domain adaptation: a cycle GAN translation approach
Lopes L, Jiao F, Xue S, Pyka T, Krieger K, Ge J, Xu Q, Fahmi R, Spottiswoode B, Soliman A, Buchert R, Brendel M, Hong J, Guan Y, Bassetti CLA, Rominger A, Zuo C, Shi K and Wu P
Dopaminergic PET to SPECT domain adaptation: a cycle GAN translation approach
Lopes L, Jiao F, Xue S, Pyka T, Krieger K, Ge J, Xu Q, Fahmi R, Spottiswoode B, Soliman A, Buchert R, Brendel M, Hong J, Guan Y, Bassetti CLA, Rominger A, Zuo C, Shi K and Wu P
Dopamine transporter imaging is routinely used in Parkinson's disease (PD) and atypical parkinsonian syndromes (APS) diagnosis. While [C]CFT PET is prevalent in Asia with a large APS database, Europe relies on [I]FP-CIT SPECT with limited APS data. Our aim was to develop a deep learning-based method to convert [C]CFT PET images to [I]FP-CIT SPECT images, facilitating multicenter studies and overcoming data scarcity to promote Artificial Intelligence (AI) advancements.
Clinical significance of quantitative assessment of right ventricular amyloid burden with [Tc]Tc-DPD SPECT/CT in transthyretin cardiac amyloidosis
Zhao M, Calabretta R, Binder P, Yu J, Jiang Z, Nitsche C, Bartko P, Rettl R, Wollenweber T, Mascherbauer K, Bondermann D, Hacker M and Li X
Clinical significance of quantitative assessment of right ventricular amyloid burden with [Tc]Tc-DPD SPECT/CT in transthyretin cardiac amyloidosis
Zhao M, Calabretta R, Binder P, Yu J, Jiang Z, Nitsche C, Bartko P, Rettl R, Wollenweber T, Mascherbauer K, Bondermann D, Hacker M and Li X
To evaluate right ventricular (RV) uptake measured by quantitative [Tc]Tc-DPD SPECT/CT to investigate its role in predicting and evaluating prognosis and therapeutic outcomes in patients with transthyretin amyloid cardiomyopathy (ATTR-CA).
Correction to: EANM perspectives for CZT SPECT in brain applications
Verger A, Cecchin D, Guedj E, Albert NL, Brendel M, Fraioli F, Tolboom N, Traub-Weidinger T, Yakushev I, Van Weehaeghe D, Fernandez PA, Garibotto V and Imbert L
Correction to: EANM perspectives for CZT SPECT in brain applications
Verger A, Cecchin D, Guedj E, Albert NL, Brendel M, Fraioli F, Tolboom N, Traub-Weidinger T, Yakushev I, Van Weehaeghe D, Fernandez PA, Garibotto V and Imbert L
DPD Quantification Correlates With Extracellular Volume and Disease Severity in Wild-Type Transthyretin Cardiac Amyloidosis
Rettl R, Calabretta R, Duca F, Kronberger C, Binder C, Willixhofer R, Poledniczek M, Hofer F, Doná C, Beitzke D, Loewe C, Nitsche C, Hengstenberg C, Badr Eslam R, Kastner J, Bergler-Klein J, Hacker M and Kammerlander AA
DPD Quantification Correlates With Extracellular Volume and Disease Severity in Wild-Type Transthyretin Cardiac Amyloidosis
Rettl R, Calabretta R, Duca F, Kronberger C, Binder C, Willixhofer R, Poledniczek M, Hofer F, Doná C, Beitzke D, Loewe C, Nitsche C, Hengstenberg C, Badr Eslam R, Kastner J, Bergler-Klein J, Hacker M and Kammerlander AA
The pathophysiological hallmark of wild-type transthyretin amyloid cardiomyopathy (ATTRwt-CM) is the deposition of amyloid within the myocardium.
Clinical development and proof of principle testing of new regenerative vascular endothelial growth factor-D therapy for refractory angina: rationale and design of the phase 2 ReGenHeart trial
Leikas AJ, Hartikainen JEK, Kastrup J, Mathur A, Gyöngyösi M, Fernández-Avilés F, Sanz-Ruiz R, Wojakowski W, Gwizdała A, Luite R, Nikkinen M, Qayyum AA, Haack-Sørensen M, Kelham M, Jones DA, Hamzaraj K, Spannbauer A, Fernández-Santos ME, Jędrzejek M, Skoczyńska A, Vartiainen N, Knuuti J, Saraste A and Ylä-Herttuala S
Clinical development and proof of principle testing of new regenerative vascular endothelial growth factor-D therapy for refractory angina: rationale and design of the phase 2 ReGenHeart trial
Leikas AJ, Hartikainen JEK, Kastrup J, Mathur A, Gyöngyösi M, Fernández-Avilés F, Sanz-Ruiz R, Wojakowski W, Gwizdała A, Luite R, Nikkinen M, Qayyum AA, Haack-Sørensen M, Kelham M, Jones DA, Hamzaraj K, Spannbauer A, Fernández-Santos ME, Jędrzejek M, Skoczyńska A, Vartiainen N, Knuuti J, Saraste A and Ylä-Herttuala S
Despite tremendous therapeutic advancements, a significant proportion of coronary artery disease patients suffer from refractory angina pectoris, that is, quality-of-life-compromising angina that is non-manageable with established pharmacological and interventional treatment options. Adenoviral vascular endothelial growth factor-D (AdVEGF-D)-encoding gene therapy (GT) holds promise for the treatment of refractory angina.
Correction to: Preclinical SPECT and PET: Joint EANM and ESMI procedure guideline for implementing an efficient quality control programme
Vanhove C, Koole M, Fragoso Costa P, Schottelius M, Mannheim J, Kuntner C, Warnock G, McDougald W, Tavares A and Bernsen M
Correction to: Preclinical SPECT and PET: Joint EANM and ESMI procedure guideline for implementing an efficient quality control programme
Vanhove C, Koole M, Fragoso Costa P, Schottelius M, Mannheim J, Kuntner C, Warnock G, McDougald W, Tavares A and Bernsen M
Recent Advances on Pt-Based Compounds for Theranostic Applications
Ferrari G, Lopez-Martinez I, Wanek T, Kuntner C and Montagner D
Recent Advances on Pt-Based Compounds for Theranostic Applications
Ferrari G, Lopez-Martinez I, Wanek T, Kuntner C and Montagner D
Since the discovery of cisplatin's antitumoral activity and its approval as an anticancer drug, significant efforts have been made to enhance its physiological stability and anticancer efficacy and to reduce its side effects. With the rapid development of targeted and personalized therapies, and the promising theranostic approach, platinum drugs have found new opportunities in more sophisticated systems. Theranostic agents combine diagnostic and therapeutic moieties in one scaffold, enabling simultaneous disease monitoring, therapy delivery, response tracking, and treatment efficacy evaluation. In these systems, the platinum core serves as the therapeutic agent, while the functionalized ligand provides diagnostic tools using various imaging techniques. This review aims to highlight the significant role of platinum-based complexes in theranostic applications, and, to the best of our knowledge, this is the first focused contribution on this type of platinum compounds. This review presents a brief introduction to the development of platinum chemotherapeutic drugs, their limitations, and resistance mechanisms. It then describes recent advancements in integrating platinum complexes with diagnostic agents for both tumor treatment and monitoring. The main body is organized into three categories based on imaging techniques: fluorescence, positron emission tomography (PET), single-photon emission computed tomography (SPECT), and magnetic resonance imaging (MRI). Finally, this review outlines promising strategies and future perspectives in this evolving field.
Recovery of cardiovascular diagnostic testing in Italy 1 year after coronavirus disease-2019 outbreak compared with other countries in Europe and worldwide: results from the International Atomic Energy Agency INCAPS COVID 2 survey
Pontone G, Bremner L, Del Torto A, Albano D, Baritussio A, Bauckneht M, Cuocolo A, Frantellizzi V, Gatti M, Gimelli A, Guglielmo M, Leccisotti L, Marcassa C, Russo V, Sciagrà R, Williams MC, Better N, Cerci R, Choi AD, Dorbala S, Hirschfeld CB, Karthikeyan G, Pascual TNB, Shaw LJ, Villines TC, Vitola J, Cohen Y, Malkovskiy E, Randazzo M, Pynda Y, Dondi M, Einstein AJ and Paez D
Recovery of cardiovascular diagnostic testing in Italy 1 year after coronavirus disease-2019 outbreak compared with other countries in Europe and worldwide: results from the International Atomic Energy Agency INCAPS COVID 2 survey
Pontone G, Bremner L, Del Torto A, Albano D, Baritussio A, Bauckneht M, Cuocolo A, Frantellizzi V, Gatti M, Gimelli A, Guglielmo M, Leccisotti L, Marcassa C, Russo V, Sciagrà R, Williams MC, Better N, Cerci R, Choi AD, Dorbala S, Hirschfeld CB, Karthikeyan G, Pascual TNB, Shaw LJ, Villines TC, Vitola J, Cohen Y, Malkovskiy E, Randazzo M, Pynda Y, Dondi M, Einstein AJ and Paez D
Recovery of cardiovascular diagnostic testing in Italy after the coronavirus disease-2019 (COVID-19) pandemic has not been quantified. The study aims to describe cardiac diagnostic procedure volumes, centres practice and protocols, and staff members' well-being 1 year after COVID-19 outbreak in Italy.
Results from a phase I study of 4--[131I]iodo-phenylalanine ([I]IPA) with external radiation therapy in patients with recurrent glioblastoma (IPAX-1)
Pichler J, Traub-Weidinger T, Spiegl K, Imamovic L, Braat AJAT, Snijders TJ, Verhoeff JJC, Flamen P, Tauchmanova L, Hayward C and Kluge A
Results from a phase I study of 4--[131I]iodo-phenylalanine ([I]IPA) with external radiation therapy in patients with recurrent glioblastoma (IPAX-1)
Pichler J, Traub-Weidinger T, Spiegl K, Imamovic L, Braat AJAT, Snijders TJ, Verhoeff JJC, Flamen P, Tauchmanova L, Hayward C and Kluge A
Glioblastoma (GBM), the most common malignant brain tumor, is associated with devastating outcomes. IPAX-1 was a multicenter, open-label, single-arm phase I study to evaluate carrier-added 4--[I]iodo-phenylalanine ([I]IPA) plus external radiation therapy (XRT) in recurrent GBM.
Teilbereich Nuklearmedizinische Therapie
Targeted radionuclide therapy for patients with central nervous system metastasis: Overlooked potential?
Le Rhun E, Albert NL, Hüllner M, Franceschi E, Galldiks N, Karschnia P, Minniti G, Weiss T, Preusser M, Ellingson BM and Weller M
Targeted radionuclide therapy for patients with central nervous system metastasis: Overlooked potential?
Le Rhun E, Albert NL, Hüllner M, Franceschi E, Galldiks N, Karschnia P, Minniti G, Weiss T, Preusser M, Ellingson BM and Weller M
Targeted radionuclide therapy is an emerging therapeutic concept for metastatic cancer that can be considered if a tumor can be delineated by nuclear medicine imaging and also targeted based on the expression of a particular target (thera-nostics). This mode of treatment can also compete with or supplement conventional radiotherapy, for example, if MRI does not fully capture the extent of the disease, including microscopic metastases. Targeted radionuclide therapy for patients with thyroid cancer, with certain somatostatin receptor 2-expressing tumors and with prostate-specific membrane antigen-expressing prostate cancer is approved, and numerous approaches of targeted radionuclide therapy for patients with metastatic cancer are in development (eg, using fibroblast activation protein as a target). Although brain metastases are rare in cancers with approved targeted radionuclide therapies, there is no a priori reason to assume that such treatments would not be effective against brain metastases if the targets are expressed and not shielded by the blood-brain barrier. Here, we discuss the current state of the art and opportunities of targeted radionuclide therapies for patients with brain and leptomeningeal metastases.
Targeted radionuclide therapy for gliomas: Emerging clinical trial landscape
Weller M, Albert NL, Galldiks N, Bink A, Preusser M, Sulman EP, Treyer V, Wen PY, Tonn JC and Le Rhun E
Targeted radionuclide therapy for gliomas: Emerging clinical trial landscape
Weller M, Albert NL, Galldiks N, Bink A, Preusser M, Sulman EP, Treyer V, Wen PY, Tonn JC and Le Rhun E
According to the new WHO classification of 2021, gliomas are a heterogeneous group of tumors with very different histology, molecular genetics, and prognoses. In addition to glioblastomas, the most common gliomas, there are also numerous less common gliomas, some of which have a very favorable prognosis. Targeted radionuclide therapy is a therapeutic option that can be attractive if a tumor can be targeted based on its molecular characteristics. It is particularly useful when tumors cannot be completely resected or when conventional imaging does not fully capture the extent of the tumor. Numerous approaches to radionuclide therapy for gliomas are in early development. The most advanced approaches for patients with gliomas in the clinic employ L-type amino acid transporter 1 as an uptake mechanism for radiolabeled amino acids or target somatostatin receptor 2 or gastrin-releasing peptide receptor. Here, we discuss the various target structures of radionuclide therapy in gliomas and provide an outlook for which glioma entities radionuclide therapy could most likely provide a therapeutic alternative.
Design and conduct of theranostic trials in neuro-oncology: Challenges and opportunities
Wen PY, Preusser M and Albert NL
Design and conduct of theranostic trials in neuro-oncology: Challenges and opportunities
Wen PY, Preusser M and Albert NL
Theranostics is a new treatment modality integrating molecular imaging with targeted radionuclide therapy. Theranostic agents have received regulatory approval for some systemic cancers and have therapeutic potential in neuro-oncology. As clinical trials are developed to evaluate the efficacy of theranostic agents in brain tumors, specific considerations will have to be considered, taking into account lessons learned from previous studies examining other treatment modalities in neuro-oncology. These include the need for molecular imaging or surgical window-of-opportunity studies to confirm adequate passage across the blood-brain barrier, optimize eligibility criteria, and selection of the most appropriate response criteria and endpoints to address issues such as pseudoprogression. This review will discuss some of the issues that should be considered when designing clinical trials for theranostic agents.
Radiopharmaceutical formulation and preliminary clinical dosimetry of [Lu]Lu-DOTA-MGS5 for application in peptide receptor radionuclide therapy
Zavvar TS, Hörmann AA, Konijnenberg M, Kraihammer M, Mair C, Kronthaler A, Joosten L, Laverman P, Gruber L, di Santo G, Decristoforo C, Virgolini I and von Guggenberg E
Radiopharmaceutical formulation and preliminary clinical dosimetry of [Lu]Lu-DOTA-MGS5 for application in peptide receptor radionuclide therapy
Zavvar TS, Hörmann AA, Konijnenberg M, Kraihammer M, Mair C, Kronthaler A, Joosten L, Laverman P, Gruber L, di Santo G, Decristoforo C, Virgolini I and von Guggenberg E
Radiolabelled minigastrin (MG) analogues targeting the cholecystokinin-2 receptor (CCK2R) have proven to be a promising approach for peptide receptor radionuclide therapy (PRRT). In this study, we report on the radiopharmaceutical development and standardization of the preparation of [Lu]Lu-DOTA-MGS5 using an automated synthesis module. Furthermore, we present the preclinical tests required to move forward towards a first therapeutic clinical trial as well as preliminary clinical dosimetry data.
High-Dose Epidermal Radionuclide Therapy with Re (Rhenium) Resin in a Patient with Multiple Actinic Keratoses
Mirzaei S and Kunstfeld R
High-Dose Epidermal Radionuclide Therapy with Re (Rhenium) Resin in a Patient with Multiple Actinic Keratoses
Mirzaei S and Kunstfeld R
High-dose epidermal radionuclide therapy using a nonsealed Re (Rhenium) resin is an alternative treatment option for nonmelanoma skin cancer. In this case study, we present the possible use of this therapy in a patient with multiple actinic keratosis (AK), which is a precancer of the skin. A 55-year-old male was presented in our department with multiple AK, located on the cheek, temporal, and frontal area, with 1, 1, 2.1, and 2.5 cm surface. Applied activity was 80, 80, 167, and 168 MBq Re with a target absorbed dose for each lesion 35 Gy at 1 mm. The treatment was well tolerated. At 17 months' follow-up, all treated area showed complete remission. There were no side effects, except mild focal hypopigmentation. This case demonstrates the high potential of epidermal radionuclide therapy with a nonsealed Re as a noninvasive, effective, and well-tolerated therapy option for patients with multiple AK, when surgery is difficult to perform or not recommended of other reasons.
Influence of dosimetry accuracy on the correlation with treatment outcome in a preliminary PSMA radiopharmaceutical therapy study
Hu J, Seifert R, Karkampouna S, Gomes CV, Xue S, Afshar-Ormieh A, Rominger A and Shi K
Influence of dosimetry accuracy on the correlation with treatment outcome in a preliminary PSMA radiopharmaceutical therapy study
Hu J, Seifert R, Karkampouna S, Gomes CV, Xue S, Afshar-Ormieh A, Rominger A and Shi K
Despite the potential of dosimetry in optimizing personalized radiopharmaceutical therapy (RPT), its limited clinical implementation impedes the development of simplified protocols for routine adoption. However, simplifications may introduce errors in dosimetry, prompting questions about their impact on clinical practice.
Peptide Receptor Radionuclide Therapy Using Y- and Lu-DOTATATE Modulating Atherosclerotic Plaque Inflammation: Longitudinal Monitoring by Ga-DOTATATE Positron Emissions Tomography/Computer Tomography
Rubinstein G, Ilhan H, Bartenstein P, Lehner S, Hacker M, Todica A, Zacherl MJ and Fischer M
Peptide Receptor Radionuclide Therapy Using Y- and Lu-DOTATATE Modulating Atherosclerotic Plaque Inflammation: Longitudinal Monitoring by Ga-DOTATATE Positron Emissions Tomography/Computer Tomography
Rubinstein G, Ilhan H, Bartenstein P, Lehner S, Hacker M, Todica A, Zacherl MJ and Fischer M
Atherosclerosis and its sequels, such as coronary artery disease and cerebrovascular stroke, still represent global health burdens. The pathogenesis of atherosclerosis consists of growing calcified plaques in the arterial wall and is accompanied by inflammatory processes, which are not entirely understood. This study aims to evaluate the effect of peptide receptor radionuclide therapy (PRRT) using Y- and Lu-DOTATATE on atherosclerotic plaque inflammation. : Atherosclerotic plaques in 57 cancer patients receiving PRRT using Y- and Lu-DOTATATE were longitudinally monitored by Ga-DOTATATE PET/CT. The target-to-background ratio (TBR) and overall vessel uptake (OVU) were measured in eight distinct arterial regions (ascending aorta, aortic arch, descending aorta, abdominal aorta, both iliac arteries, and both carotid arteries) to monitor calcified plaques. PET/CT analysis shows a positive correlation between calcified plaque scores and the Ga-DOTATATE overall vessel uptake (OVU) in cancer patients. After PRRT, an initially high OVU was observed to decrease in the therapy group compared to the control group. An excellent correlation could be shown for each target-to-background ratio (TBR) to the OVU, especially the ascending aorta. The ascending aorta could present a future reference for estimating generalized atherosclerotic inflammatory processes. PRRT might represent a therapeutic approach to modulating atherosclerotic plaques.
Joint EANM/EANO/RANO/SNMMI practice guideline/procedure standards for diagnostics and therapy (theranostics) of meningiomas using radiolabeled somatostatin receptor ligands: version 1.0
Albert NL, Preusser M, Traub-Weidinger T, Tolboom N, Law I, Palmer JD, Guedj E, Furtner J, Fraioli F, Huang RY, Johnson DR, Deroose CM, Herrmann K, Vogelbaum M, Chang S, Tonn JC, Weller M, Wen PY, van den Bent MJ, Verger A, Ivanidze J and Galldiks N
Joint EANM/EANO/RANO/SNMMI practice guideline/procedure standards for diagnostics and therapy (theranostics) of meningiomas using radiolabeled somatostatin receptor ligands: version 1.0
Albert NL, Preusser M, Traub-Weidinger T, Tolboom N, Law I, Palmer JD, Guedj E, Furtner J, Fraioli F, Huang RY, Johnson DR, Deroose CM, Herrmann K, Vogelbaum M, Chang S, Tonn JC, Weller M, Wen PY, van den Bent MJ, Verger A, Ivanidze J and Galldiks N
To provide practice guideline/procedure standards for diagnostics and therapy (theranostics) of meningiomas using radiolabeled somatostatin receptor (SSTR) ligands.
Translating the theranostic concept to neuro-oncology: disrupting barriers
Albert NL, Le Rhun E, Minniti G, Mair MJ, Galldiks N, Tolboom N, Jakola AS, Niyazi M, Smits M, Verger A, Cicone F, Weller M, Preusser M and
Translating the theranostic concept to neuro-oncology: disrupting barriers
Albert NL, Le Rhun E, Minniti G, Mair MJ, Galldiks N, Tolboom N, Jakola AS, Niyazi M, Smits M, Verger A, Cicone F, Weller M, Preusser M and
Theranostics integrate molecular imaging and targeted radionuclide therapy for personalised cancer therapy. Theranostic treatments have shown meaningful efficacy in randomised clinical trials and are approved for clinical use in prostate cancer and neuroendocrine tumours. Brain tumours represent an unmet clinical need and theranostics might offer effective treatment options, although specific issues need to be considered for clinical development. In this Policy Review, we discuss opportunities and challenges of developing targeted radionuclide therapies for the treatment of brain tumours including glioma, meningioma, and brain metastasis. The rational choice of molecular treatment targets is highlighted, including the potential relevance of different types of targeted radionuclide therapeutics, and the role of the blood-brain barrier and blood-tumour barrier. Furthermore, we discuss considerations for effective clinical trial design and conduct, as well as logistical and regulatory challenges for implementation of radionuclide therapies into neuro-oncological practice. Rational development will foster successful translation of the theranostic concept to brain tumours.
Novel Detection of Pleomorphic Adenomas via Analysis of Ga-DOTATOC PET/CT Imaging
Johnson F, Kloppenburg M, Hofauer B, Wollenberg B, Hoch CC, Stögbauer F, Haller B, Knopf A, Strassen U and Notohamiprodjo S
Novel Detection of Pleomorphic Adenomas via Analysis of Ga-DOTATOC PET/CT Imaging
Johnson F, Kloppenburg M, Hofauer B, Wollenberg B, Hoch CC, Stögbauer F, Haller B, Knopf A, Strassen U and Notohamiprodjo S
Currently, the diagnosis of salivary gland tumors using imaging techniques is unreliable.