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3. Position paper to facilitate patient access to radiopharmaceuticals: considerations for a suitable pharmaceutical regulatory framework

Author

Korde, A, Patt, M, Selivanova, S, Scott, A, Hesselmann, R, Kiss, O, Ramamoorthy, N, Todde, S, Rubow, S, Gwaza, L, Lyashchenko, S, Andersson, J, Hockley, B, Kaslival, R, Decristoforo, C, Korde A., Patt M., Selivanova S. V., Scott A. M., Hesselmann R., Kiss O., Ramamoorthy N., Todde S., Rubow S. M., Gwaza L., Lyashchenko S., Andersson J., Hockley B., Kaslival R., Decristoforo C., Korde, A, Patt, M, Selivanova, S, Scott, A, Hesselmann, R, Kiss, O, Ramamoorthy, N, Todde, S, Rubow, S, Gwaza, L, Lyashchenko, S, Andersson, J, Hockley, B, Kaslival, R, Decristoforo, C, Korde A., Patt M., Selivanova S. V., Scott A. M., Hesselmann R., Kiss O., Ramamoorthy N., Todde S., Rubow S. M., Gwaza L., Lyashchenko S., Andersson J., Hockley B., Kaslival R., and Decristoforo C.

Abstract

Background: Nuclear medicine has made enormous progress in the past decades. However, there are still significant inequalities in patient access among different countries, which could be mitigated by improving access to and availability of radiopharmaceuticals. Main body: This paper summarises major considerations for a suitable pharmaceutical regulatory framework to facilitate patient access to radiopharmaceuticals. These include the distinct characteristics of radiopharmaceuticals which require dedicated regulations, considering the impact of the variable complexity of radiopharmaceutical preparation, personnel requirements, manufacturing practices and quality assurance, regulatory authority interfaces, communication and training, as well as marketing authorisation procedures to ensure availability of radiopharmaceuticals. Finally, domestic and regional supply to ensure patient access via alternative regulatory pathways, including in-house production of radiopharmaceuticals, is described, and an outlook on regulatory challenges faced by new developments, such as the use of alpha emitters, is provided. Conclusions: All these considerations are an outcome of a dedicated Technical Meeting organised by the IAEA in 2023 and represent the views and opinions of experts in the field, not those of any regulatory authorities.

Published
2024

4. Position Paper to facilitate patient access to radiopharmaceuticals - considerations for a suitable pharmaceutical regulatory framework

Author

Korde, A., Patt, M., Selivanova, S., Scott, A., Hesselmann, R., (0000-0001-7431-0026) Kiß, O., Ramamoorthy, N., Todde, S., Rubow, S., Gwaza, L., Lyashchenko, S., Andersson, J., Hockley, B., Kaslival, R., Decristoforo, C., Korde, A., Patt, M., Selivanova, S., Scott, A., Hesselmann, R., (0000-0001-7431-0026) Kiß, O., Ramamoorthy, N., Todde, S., Rubow, S., Gwaza, L., Lyashchenko, S., Andersson, J., Hockley, B., Kaslival, R., and Decristoforo, C.

Abstract

Nuclear medicine has made enormous progress in the past decades. However, there are still significant inequalities in patient access among different countries, which could be mitigated by a suitable pharmaceutical regulatory framework and associated guidelines. This paper summarizes major considerations for a suitable pharmaceutical regulatory framework to facilitate patient access to radiopharmaceuticals. These include the distinct characteristics of radiopharmaceuticals advocating dedicated regulations, the impact of variable complexity of radiopharmaceutical preparation, personnel requirements, manufacturing practices and quality assurance, regulatory authorities interfaces, communication and training, as well as marketing authorization procedures to ensure availability of radiopharmaceuticals. Finally domestic and regional supply to ensure patient access via alternative regulatory pathways, including in-house production of radiopharmaceuticals, is described and an outlook on regulatory challenges faced by new developments, such as the use of alpha emitters, is provided. All these considerations are an outcome of a dedicated Technical Meeting organized by the IAEA in 2023.

Published
2024

5. Electric field-driven coherent spin reorientation of optically generated electron spin packets in InGaAs

Author

Kuhlen, S., Schmalbuch, K., Hagedorn, M., Schlammes, P., Patt, M., Lepsa, M., Güntherodt, G., and Beschoten, B.

Subjects
Condensed Matter - Materials Science, Condensed Matter - Mesoscale and Nanoscale Physics
Abstract

Full electric-field control of spin orientations is one of the key tasks in semiconductor spintronics. We demonstrate that electric field pulses can be utilized for phase-coherent +/- pi spin rotation of optically generated electron spin packets in InGaAs epilayers detected by time-resolved Faraday rotation. Through spin-orbit interaction, the electric-field pulses act as local magnetic field pulses (LMFP). By the temporal control of the LMFP, we can turn on and off electron spin precession and thereby rotate the spin direction into arbitrary orientations in a 2-dimensional plane. Furthermore, we demonstrate a spin echo-type spin drift experiment and find an unexpected partial spin rephasing, which is evident by a doubling of the spin dephasing time., Comment: 10 pages, 4 figures

Published
2011
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7. EANM guideline on quality risk management for radiopharmaceuticals

Author

Gillings, N, Hjelstuen, O, Behe, M, Decristoforo, C, Elsinga, P, Ferrari, V, Kiss, O, Kolenc, P, Koziorowski, J, Laverman, P, Mindt, T, Ocak, M, Patt, M, Todde, S, Walte, A, Gillings N., Hjelstuen O., Behe M., Decristoforo C., Elsinga P. H., Ferrari V., Kiss O. C., Kolenc P., Koziorowski J., Laverman P., Mindt T. L., Ocak M., Patt M., Todde S., Walte A., Gillings, N, Hjelstuen, O, Behe, M, Decristoforo, C, Elsinga, P, Ferrari, V, Kiss, O, Kolenc, P, Koziorowski, J, Laverman, P, Mindt, T, Ocak, M, Patt, M, Todde, S, Walte, A, Gillings N., Hjelstuen O., Behe M., Decristoforo C., Elsinga P. H., Ferrari V., Kiss O. C., Kolenc P., Koziorowski J., Laverman P., Mindt T. L., Ocak M., Patt M., Todde S., and Walte A.

Abstract

This document is intended as a supplement to the EANM “Guidelines on current Good Radiopharmacy Practice (cGRPP)” issued by the Radiopharmacy Committee of the EANM (Gillings et al. in EJNMMI Radiopharm Chem. 6:8, 2021). The aim of the EANM Radiopharmacy Committee is to provide a document that describes how to manage risks associated with small-scale “in-house” preparation of radiopharmaceuticals, not intended for commercial purposes or distribution.

Published
2022

8. Dopamine D1 receptor availability in Gilles de la Tourette syndrome (GTS): A C-11-SCH23390 PET study

Author

Rullmann, M., additional, Gkotsoulias, D., additional, Schmitt, S., additional, Fremer, C., additional, Klages, C., additional, Hartung, K., additional, Bujanow, A., additional, Zientek, F., additional, Messerschmidt, K., additional, Patt, M., additional, Sabri, O., additional, Müller-Vahl, K. R., additional, Möller, H., additional, and Barthel, H., additional

Published
2023
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9. Amyloid-Bildgebung in der Differentialdiagnostik zwischen Alzheimer-bedingter Depression und Pseudodemenz bei Depression: Eine neue Indikation?

Author

Leonhardi, J., additional, Barthel, H., additional, Speerforck, S., additional, Dietzel, J., additional, Schröter, M., additional, Saur, D., additional, Tiepolt, S., additional, Rullmann, M., additional, Patt, M., additional, Claßen, J., additional, Schomerus, G., additional, and Sabri, O., additional

Published
2023
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11. Additive value of [18F]PI-2620 perfusion imaging in progressive supranuclear palsy and corticobasal syndrome

Author

Katzdobler, S, Nitschmann, A, Barthel, H, Bischof, G, Beyer, L, Marek, K, Song, M, Wagemann, O, Palleis, C, Weidinger, E, Nack, A, Fietzek, U, Kurz, C, Haeckert, J, Stapf, T, Ferschmann, C, Scheifele, M, Eckenweber, F, Biechele, G, Franzmeier, N, Dewenter, A, Schoenecker, S, Saur, D, Schroeter, ML, Rumpf, J-J, Rullmann, M, Schildan, A, Patt, M, Stephens, AW, van Eimeren, T, Neumaier, B, Drzezga, A, Danek, A, Classen, J, Buerger, K, Janowitz, D, Rauchmann, B-S, Stoecklein, S, Perneczky, R, Schoeberl, F, Zwergal, A, Hoeglinger, GU, Bartenstein, P, Villemagne, V, Seibyl, J, Sabri, O, Levin, J, Brendel, M, Katzdobler, S, Nitschmann, A, Barthel, H, Bischof, G, Beyer, L, Marek, K, Song, M, Wagemann, O, Palleis, C, Weidinger, E, Nack, A, Fietzek, U, Kurz, C, Haeckert, J, Stapf, T, Ferschmann, C, Scheifele, M, Eckenweber, F, Biechele, G, Franzmeier, N, Dewenter, A, Schoenecker, S, Saur, D, Schroeter, ML, Rumpf, J-J, Rullmann, M, Schildan, A, Patt, M, Stephens, AW, van Eimeren, T, Neumaier, B, Drzezga, A, Danek, A, Classen, J, Buerger, K, Janowitz, D, Rauchmann, B-S, Stoecklein, S, Perneczky, R, Schoeberl, F, Zwergal, A, Hoeglinger, GU, Bartenstein, P, Villemagne, V, Seibyl, J, Sabri, O, Levin, J, and Brendel, M

Abstract

PURPOSE: Early after [18F]PI-2620 PET tracer administration, perfusion imaging has potential for regional assessment of neuronal injury in neurodegenerative diseases. This is while standard late-phase [18F]PI-2620 tau-PET is able to discriminate the 4-repeat tauopathies progressive supranuclear palsy and corticobasal syndrome (4RTs) from disease controls and healthy controls. Here, we investigated whether early-phase [18F]PI-2620 PET has an additive value for biomarker based evaluation of 4RTs. METHODS: Seventy-eight patients with 4RTs (71 ± 7 years, 39 female), 79 patients with other neurodegenerative diseases (67 ± 12 years, 35 female) and twelve age-matched controls (69 ± 8 years, 8 female) underwent dynamic (0-60 min) [18F]PI-2620 PET imaging. Regional perfusion (0.5-2.5 min p.i.) and tau load (20-40 min p.i.) were measured in 246 predefined brain regions [standardized-uptake-value ratios (SUVr), cerebellar reference]. Regional SUVr were compared between 4RTs and controls by an ANOVA including false-discovery-rate (FDR, p < 0.01) correction. Hypoperfusion in resulting 4RT target regions was evaluated at the patient level in all patients (mean value - 2SD threshold). Additionally, perfusion and tau pattern expression levels were explored regarding their potential discriminatory value of 4RTs against other neurodegenerative disorders, including validation in an independent external dataset (n = 37), and correlated with clinical severity in 4RTs (PSP rating scale, MoCA, activities of daily living). RESULTS: Patients with 4RTs had significant hypoperfusion in 21/246 brain regions, most dominant in thalamus, caudate nucleus, and anterior cingulate cortex, fitting to the topology of the 4RT disease spectrum. However, single region hypoperfusion was not specific regarding the discrimination of patients with 4RTs against patients with other neurodegenerative diseases. In contrast, perfusion pattern expression showed promise for discrimination of patients with 4RTs from

Published
2023

12. Highlight selection of radiochemistry and radiopharmacy developments by editorial board

Author

Kiss, O.C., Scott, P.J.H., Behe, M., Penuelas, I., Passchier, J., Rey, A., Patt, M., Aime, S., Jalilian, A., Laverman, P., Cheng, Z., Chauvet, A.F., Engle, J., Cleeren, F., Zhu, H., Vercouillie, J., Dam, Michael van, Zhang, M.R., Perk, Lars, Guillet, B., Alves, F., Kiss, O.C., Scott, P.J.H., Behe, M., Penuelas, I., Passchier, J., Rey, A., Patt, M., Aime, S., Jalilian, A., Laverman, P., Cheng, Z., Chauvet, A.F., Engle, J., Cleeren, F., Zhu, H., Vercouillie, J., Dam, Michael van, Zhang, M.R., Perk, Lars, Guillet, B., and Alves, F.

Abstract

Contains fulltext : 294699.pdf (Publisher’s version ) (Open Access), BACKGROUND: The Editorial Board of EJNMMI Radiopharmacy and Chemistry releases a biannual highlight commentary to update the readership on trends in the field of radiopharmaceutical development. MAIN BODY: This selection of highlights provides commentary on 21 different topics selected by each coauthoring Editorial Board member addressing a variety of aspects ranging from novel radiochemistry to first-in-human application of novel radiopharmaceuticals. CONCLUSION: Trends in radiochemistry and radiopharmacy are highlighted. Hot topics cover the entire scope of EJNMMI Radiopharmacy and Chemistry, demonstrating the progress in the research field, and include new PET-labelling methods for (11)C and (18)F, the importance of choosing the proper chelator for a given radioactive metal ion, implications of total body PET on use of radiopharmaceuticals, legislation issues and radionuclide therapy including the emerging role of (161)Tb.

Published
2023

14. Highlight selection of radiochemistry and radiopharmacy developments by editorial board

Author

(0000-0001-7431-0026) Kiß, O., Scott, P., Behe, M., Penuelas, I., Passchier, J., Rey, A., Patt, M., Aime, S., Jalilian, A., Laverman, P., Cheng, Z., Faivre Chauvet, A., Engle, J., Cleeren, F., Zhu, H., Vercouille, J., Dam, M., Zhang, M.-R., Perk, L., Guillet, B., Alves, F., (0000-0001-7431-0026) Kiß, O., Scott, P., Behe, M., Penuelas, I., Passchier, J., Rey, A., Patt, M., Aime, S., Jalilian, A., Laverman, P., Cheng, Z., Faivre Chauvet, A., Engle, J., Cleeren, F., Zhu, H., Vercouille, J., Dam, M., Zhang, M.-R., Perk, L., Guillet, B., and Alves, F.

Abstract

Background: The Editorial Board of EJNMMI Radiopharmacy and Chemistry releases a biannual highlight commentary to update the readership on trends in the field of radiopharmaceutical development. Main Body: This selection of highlights provides commentary on 21 different topics selected by each coauthoring Editorial Board member addressing a variety of aspects ranging from novel radiochemistry to first-in-human application of novel radiopharmaceuticals. Conclusion: Trends in radiochemistry and radiopharmacy are highlighted. Hot topics cover the entire scope of EJNMMI Radiopharmacy and Chemistry, demonstrating the progress in the research field, and include new PET-labelling methods for 11C and 18F, the importance of choosing the proper chelator for a given radioactive metal ion, implications of total body PET on use of radiopharmaceuticals, legislation issues and radionuclide therapy including the emerging role of 161Tb.

Published
2023

17. Guideline on current good radiopharmacy practice (cGRPP) for the small-scale preparation of radiopharmaceuticals

Author

Gillings, N, Hjelstuen, O, Ballinger, J, Behe, M, Decristoforo, C, Elsinga, P, Ferrari, V, Peitl, P, Koziorowski, J, Laverman, P, Mindt, T, Neels, O, Ocak, M, Patt, M, Todde, S, Gillings N., Hjelstuen O., Ballinger J., Behe M., Decristoforo C., Elsinga P., Ferrari V., Peitl P. K., Koziorowski J., Laverman P., Mindt T. L., Neels O., Ocak M., Patt M., Todde S., Gillings, N, Hjelstuen, O, Ballinger, J, Behe, M, Decristoforo, C, Elsinga, P, Ferrari, V, Peitl, P, Koziorowski, J, Laverman, P, Mindt, T, Neels, O, Ocak, M, Patt, M, Todde, S, Gillings N., Hjelstuen O., Ballinger J., Behe M., Decristoforo C., Elsinga P., Ferrari V., Peitl P. K., Koziorowski J., Laverman P., Mindt T. L., Neels O., Ocak M., Patt M., and Todde S.

Abstract

This guideline on current good radiopharmacy practice (cGRPP) for small-scale preparation of radiopharmaceuticals represents the view of the Radiopharmacy Committee of the European Association of Nuclear Medicine (EANM). The guideline is laid out in the format of the EU Good Manufacturing Practice (GMP) guidelines as defined in EudraLex volume 4. It is intended for non-commercial sites such as hospital radiopharmacies, nuclear medicine departments, research PET centres and in general any healthcare establishments. In the first section, general aspects which are applicable to all levels of operations are discussed. The second section discusses the preparation of small-scale radiopharmaceuticals (SSRP) using licensed generators and kits. Finally, the third section goes into the more complex preparation of SSRP from non-licensed starting materials, often requiring a purification step and sterile filtration. The intention is that the guideline will assist radiopharmacies in the preparation of diagnostic and therapeutic SSRP’s safe for human administration.

Published
2021

18. Highlight selection of radiochemistry and radiopharmacy developments by editorial board

Author

Aime, S, Al-Qahtani, M, Behe, M, Bormans, G, Carlucci, G, Dasilva, J, Decristoforo, C, Duatti, A, Elsinga, P, Kopka, K, Li, X, Liu, Z, Mach, R, Middel, O, Passchier, J, Patt, M, Penuelas, I, Rey, A, Scott, P, Todde, S, Toyohara, J, Vugts, D, Yang, Z, Aime S., Al-Qahtani M., Behe M., Bormans G., Carlucci G., DaSilva J. N., Decristoforo C., Duatti A., Elsinga P. H., Kopka K., Li X. -G., Liu Z., Mach R. H., Middel O., Passchier J., Patt M., Penuelas I., Rey A., Scott P. J. H., Todde S., Toyohara J., Vugts D., Yang Z., Aime, S, Al-Qahtani, M, Behe, M, Bormans, G, Carlucci, G, Dasilva, J, Decristoforo, C, Duatti, A, Elsinga, P, Kopka, K, Li, X, Liu, Z, Mach, R, Middel, O, Passchier, J, Patt, M, Penuelas, I, Rey, A, Scott, P, Todde, S, Toyohara, J, Vugts, D, Yang, Z, Aime S., Al-Qahtani M., Behe M., Bormans G., Carlucci G., DaSilva J. N., Decristoforo C., Duatti A., Elsinga P. H., Kopka K., Li X. -G., Liu Z., Mach R. H., Middel O., Passchier J., Patt M., Penuelas I., Rey A., Scott P. J. H., Todde S., Toyohara J., Vugts D., and Yang Z.

Abstract

Background: The Editorial Board of EJNMMI Radiopharmacy and Chemistry releases a biyearly highlight commentary to update the readership on trends in the field of radiopharmaceutical development. Results: This commentary of highlights has resulted in 23 different topics selected by each member of the Editorial Board addressing a variety of aspects ranging from novel radiochemistry to first in man application of novel radiopharmaceuticals. Conclusion: Trends in radiochemistry and radiopharmacy are highlighted demonstrating the progress in the research field being the scope of EJNMMI Radiopharmacy and Chemistry.

Published
2021

21. EANM Guideline on the validation of analytical methods for radiopharmaceuticals

Author

Gillings, N, Todde, S, Behe, M, Decristoforo, C, Elsinga, P, Ferrari, V, Hjelstuen, O, Kolenc Peitl, P, Koziorowski, J, Laverman, P, Mindt, T, Ocak, M, Patt, M, Mindt, TL, Patt, M., Gillings, N, Todde, S, Behe, M, Decristoforo, C, Elsinga, P, Ferrari, V, Hjelstuen, O, Kolenc Peitl, P, Koziorowski, J, Laverman, P, Mindt, T, Ocak, M, Patt, M, Mindt, TL, and Patt, M.

Abstract

Background: To fulfil good manufacturing requirements, analytical methods for the analysis of pharmaceuticals for human and vetinary use must be validated. The International Conference on Harmonization of Technical Requirements for Registration of Pharmaceuticals for Human Use (ICH) has published guidance documents on the requirements for such validation activities and these have been adopted by the European Medicines Agency, The U.S. Food and Drug Administration (FDA) and other regulatory bodies. These guidance documents do not, however, fully address all the specific tests required for the analysis of radiopharmaceuticals. This guideline attempts to rectify this shortcoming, by recommending approaches to validate such methods. Results: Recommedations for the validation of analytical methods which are specific for radiopharmaceutials are presented in this guideline, along with two practical examples. Conclusions: In order to comply with good manufacturing practice, analytical methods for radiopharmaceuticals for human use should be validated.

Published
2020

22. Subcortical tau-accumulation predicts neuronal dysfunction in the cortex based on functional connectivity in 4R-tauopathies

Author

Roemer, SN, Franzmeier, N, Katzdobler, S, Nitschmann, A, Barthel, H, Bischof, GN, Beyer, L, Marek, K, Song, M, Wagemann, O, Palleis, C, Nack, A, Fietzek, U, Kurz, C, Haeckert, J, Stapf, T, Ferschmann, C, Scheifele, M, Eckenweber, F, Biechele, G, Biel, D, Dewenter, A, Steward, A, Schoenecker, S, Saur, D, Schroeter, ML, Rumpf, JJ, Rullmann, M, Schildan, A, Patt, M, Stephens, AW, van Eimeren, T, Drzezga, A, Danek, A, Classen, J, Bürger, K, Janowitz, D, Rauchmann, BS, Stöcklein, S, Perneczky, R, Schoeberl, F, Zwergal, A, Bartenstein, P, Neumaier, B, Villemagne, VL, Seibyl, J, Sabri, O, Levin, J, Brendel, M, Höglinger, G, Roemer, SN, Franzmeier, N, Katzdobler, S, Nitschmann, A, Barthel, H, Bischof, GN, Beyer, L, Marek, K, Song, M, Wagemann, O, Palleis, C, Nack, A, Fietzek, U, Kurz, C, Haeckert, J, Stapf, T, Ferschmann, C, Scheifele, M, Eckenweber, F, Biechele, G, Biel, D, Dewenter, A, Steward, A, Schoenecker, S, Saur, D, Schroeter, ML, Rumpf, JJ, Rullmann, M, Schildan, A, Patt, M, Stephens, AW, van Eimeren, T, Drzezga, A, Danek, A, Classen, J, Bürger, K, Janowitz, D, Rauchmann, BS, Stöcklein, S, Perneczky, R, Schoeberl, F, Zwergal, A, Bartenstein, P, Neumaier, B, Villemagne, VL, Seibyl, J, Sabri, O, Levin, J, Brendel, M, and Höglinger, G

Abstract

Background 4‐repeat (4R) tauopathies are neurodegenerative diseases characterized by cerebral accumulation of 4R tau pathology. The most prominent 4R‐tauopathies are progressive‐supranuclear‐palsy (PSP) and corticobasal‐syndrome (CBS) characterized by tau accumulation in subcortical nuclei as well as cortical neuronal dysfunction, as shown by PET‐assessed hypoperfusion and glucose hypometabolism. Yet, there is a spatial mismatch between subcortical tau deposition patterns and cortical neuronal dysfunction and it is unclear how these two pathological brain changes are interrelated. Here, we hypothesized that subcortical tau pathology induces diaschisis‐like neuronal dysfunction in functionally connected cortical regions. Method We included 47 patients with clinically diagnosed PSP or CBS who underwent structural MRI and 18F‐PI‐2620 tau‐PET. PI‐2620 PET was recorded using a dynamic one‐shot, two‐stop acquisition protocol, to determine an early 0.5‐2.5min post‐tracer‐injection perfusion window for assessing cortical neuroinjury in 200 cortical ROIs of the Schaefer atlas, as well as a 20‐40min post‐tracer‐injection window to determine 4R‐tau load in 32 subcortical ROIs of the TIAN atlas. We determined tau epicenters as 10% of subcortical ROIs with highest tau‐PET, and assessed the connectivity of tau epicenters to cortical ROIs using an age‐matched 3T resting‐state fMRI template derived from 69 healthy elderly. Using linear regression, we assessed whether i) higher subcortical tau‐PET was associated with overall reduced cortical perfusion and ii) whether cortical hypoperfusion was observed preferentially in regions closely connected to subcortical tau epicenters. Result As hypothesized, higher subcortical tau‐PET was associated with lower cortical perfusion (R=‐0,37, p‐value: <0,011, Fig.1). Using group‐average tau‐PET and perfusion‐PET, we found that the seed‐based connectivity pattern of subcortical tau epicenters predicted cortical perfusion patterns, whe

Published
2022

23. EANM guideline on quality risk management for radiopharmaceuticals

Author

Gillings, N., Hjelstuen, O., Behe, M., Decristoforo, C., Elsinga, P.H., Ferrari, V., Kiss, O.C., Kolenc, P., Koziorowski, J., Laverman, P., Mindt, T.L., Ocak, M., Patt, M., Todde, S., Walte, A., Gillings, N., Hjelstuen, O., Behe, M., Decristoforo, C., Elsinga, P.H., Ferrari, V., Kiss, O.C., Kolenc, P., Koziorowski, J., Laverman, P., Mindt, T.L., Ocak, M., Patt, M., Todde, S., and Walte, A.

Abstract

Contains fulltext : 283308.pdf (Publisher’s version ) (Open Access), This document is intended as a supplement to the EANM "Guidelines on current Good Radiopharmacy Practice (cGRPP)" issued by the Radiopharmacy Committee of the EANM (Gillings et al. in EJNMMI Radiopharm Chem. 6:8, 2021). The aim of the EANM Radiopharmacy Committee is to provide a document that describes how to manage risks associated with small-scale "in-house" preparation of radiopharmaceuticals, not intended for commercial purposes or distribution.

Published
2022

24. Multicenter 18F-PI-2620 PET for In Vivo Braak Staging of Tau Pathology in Alzheimer's Disease

Author

Rullmann, M, Brendel, M, Schroeter, ML, Saur, D, Levin, J, Perneczky, RG, Tiepolt, S, Patt, M, Mueller, A, Villemagne, VL, Classen, J, Stephens, AW, Sabri, O, Barthel, H, Rullmann, M, Brendel, M, Schroeter, ML, Saur, D, Levin, J, Perneczky, RG, Tiepolt, S, Patt, M, Mueller, A, Villemagne, VL, Classen, J, Stephens, AW, Sabri, O, and Barthel, H

Abstract

Tau aggregates accumulate in the Alzheimer's disease (AD) brain according to the established Braak staging scheme and spread from transentorhinal over limbic regions to the neocortex. To impact the management of AD patients, an in vivo tool for tau Braak staging is needed. First-generation tau tracers have limited performance in detecting early stages of tau. Therefore, we tested the corresponding capability of the next-generation tau tracer, 18F-PI-2620. We analyzed 18F-PI-2620 multicenter PET data from 37 beta-amyloid-positive AD dementia patients and those from 26 healthy controls. We applied kinetic modeling of the 0-60 min p.i. PET data using MRTM2 with the lower cerebellum as the reference region to extract Braak stage-dependent distribution volume ratios, whereas controls were used to define Braak stage PET positivity thresholds. Stage-dependent PET positivity widely followed the Braak scheme (except Braak stage III) presenting descending frequency of PET positivity from Braak I (43%), II (38%), III (49%), IV (35%), V (30%) to VI (14%). A strictly hierarchical model was met by 64% of AD dementia cases. Nineteen percent showed a hippocampal sparing tauopathy pattern. Thus, we could assign 87% to the six-stage hierarchical Braak model including tauopathy variants. 18F-PI-2620 PET appears to be able to perform Braak tau staging of AD in vivo.

Published
2022

25. Tau deposition patterns are associated with functional connectivity in primary tauopathies

Author

Franzmeier, N, Brendel, M, Beyer, L, Slemann, L, Kovacs, GG, Arzberger, T, Kurz, C, Respondek, G, Lukic, MJ, Biel, D, Rubinski, A, Frontzkowski, L, Hummel, S, Muller, A, Finze, A, Palleis, C, Joseph, E, Weidinger, E, Katzdobler, S, Song, M, Biechele, G, Kern, M, Scheifele, M, Rauchmann, B-S, Perneczky, R, Rullman, M, Patt, M, Schildan, A, Barthel, H, Sabri, O, Rumpf, JJ, Schroeter, ML, Classen, J, Villemagne, V, Seibyl, J, Stephens, AW, Lee, EB, Coughlin, DG, Giese, A, Grossman, M, McMillan, CT, Gelpi, E, Molina-Porcel, L, Compta, Y, van Swieten, JC, Laat, LD, Troakes, C, Al-Sarraj, S, Robinson, JL, Xie, SX, Irwin, DJ, Roeber, S, Herms, J, Simons, M, Bartenstein, P, Lee, VM, Trojanowski, JQ, Levin, J, Hoeglinger, G, Ewers, M, Franzmeier, N, Brendel, M, Beyer, L, Slemann, L, Kovacs, GG, Arzberger, T, Kurz, C, Respondek, G, Lukic, MJ, Biel, D, Rubinski, A, Frontzkowski, L, Hummel, S, Muller, A, Finze, A, Palleis, C, Joseph, E, Weidinger, E, Katzdobler, S, Song, M, Biechele, G, Kern, M, Scheifele, M, Rauchmann, B-S, Perneczky, R, Rullman, M, Patt, M, Schildan, A, Barthel, H, Sabri, O, Rumpf, JJ, Schroeter, ML, Classen, J, Villemagne, V, Seibyl, J, Stephens, AW, Lee, EB, Coughlin, DG, Giese, A, Grossman, M, McMillan, CT, Gelpi, E, Molina-Porcel, L, Compta, Y, van Swieten, JC, Laat, LD, Troakes, C, Al-Sarraj, S, Robinson, JL, Xie, SX, Irwin, DJ, Roeber, S, Herms, J, Simons, M, Bartenstein, P, Lee, VM, Trojanowski, JQ, Levin, J, Hoeglinger, G, and Ewers, M

Abstract

Tau pathology is the main driver of neuronal dysfunction in 4-repeat tauopathies, including cortico-basal degeneration and progressive supranuclear palsy. Tau is assumed to spread prion-like across connected neurons, but the mechanisms of tau propagation are largely elusive in 4-repeat tauopathies, characterized not only by neuronal but also by astroglial and oligodendroglial tau accumulation. Here, we assess whether connectivity is associated with 4R-tau deposition patterns by combining resting-state fMRI connectomics with both 2nd generation 18F-PI-2620 tau-PET in 46 patients with clinically diagnosed 4-repeat tauopathies and post-mortem cell-type-specific regional tau assessments from two independent progressive supranuclear palsy patient samples (n = 97 and n = 96). We find that inter-regional connectivity is associated with higher inter-regional correlation of both tau-PET and post-mortem tau levels in 4-repeat tauopathies. In regional cell-type specific post-mortem tau assessments, this association is stronger for neuronal than for astroglial or oligodendroglial tau, suggesting that connectivity is primarily associated with neuronal tau accumulation. Using tau-PET we find further that patient-level tau patterns are associated with the connectivity of subcortical tau epicenters. Together, the current study provides combined in vivo tau-PET and histopathological evidence that brain connectivity is associated with tau deposition patterns in 4-repeat tauopathies.

Published
2022

26. Status-Quo-Erhebung zur Zyklotron-Infrastruktur für die Nuklearmedizin und Radiopharmazie in Deutschland, Österreich und der Schweiz (D-A-CH)

Author

Zippel, C., Ermert, J., Patt, M., Gildehaus, F. J., Ross, T., Reischl, G., Kuwert, T., Solbach, C., Neumaier, B., (0000-0001-7431-0026) Kiß, O., Mitterhauser, M., Wadsak, W., Schibli, R., (0000-0003-4846-1271) Kopka, K., Zippel, C., Ermert, J., Patt, M., Gildehaus, F. J., Ross, T., Reischl, G., Kuwert, T., Solbach, C., Neumaier, B., (0000-0001-7431-0026) Kiß, O., Mitterhauser, M., Wadsak, W., Schibli, R., and (0000-0003-4846-1271) Kopka, K.

Abstract

Zyklotrone bilden als Ressource medizinischer Radionuklide eine zentrale Infrastruktur für die Entwicklung neuer und die Produktion klinisch etablierter Radiotracer zur molekularen Hybridbildgebung. Da die letzte umfassende Veröffentlichung zu Zyklotronen ca. 15 Jahre alt ist, wurde eine Statuserhebung zu den für die Nuklearmedizin und Radiopharmazie in Deutschland, Österreich und der Schweiz (D-A-CH-Länder) betriebenen Zyklotronen angestrebt.

Published
2022

27. EANM Position on the In-House Preparation of Radiopharmaceuticals

Author

Hendrikse, H., (0000-0001-7431-0026) Kiß, O., Kunikowska, J., Wadsak, W., Decristoforo, C., Patt, M., Hendrikse, H., (0000-0001-7431-0026) Kiß, O., Kunikowska, J., Wadsak, W., Decristoforo, C., and Patt, M.

Abstract

The daily clinical practice in Nuclear Medicine makes use of radiopharmaceuticals that either are obtained from external commercial suppliers or prepared in-house for immediate use. The latter are usually non-commercial preparations that represent the major source of radiopharmaceuticals for essential routine Nuclear Medicine practices for both diagnostic and therapeutic applications. According to European legislation, namely directive 2001/83/EC, radiopharmaceuticals that are commercially distributed must have a marketing authorization (MA) to be placed on the market. The availability of this type of finished radiopharmaceutical products with MA ready to use is limited due to different reasons: one is the very short half-life or shelf life, which limits the shipment of these radiopharmaceuticals from external sources. In addition, the market potential for radiopharmaceuticals that are used in rare clinical indications is limited to be financially attractive for pharmaceutical industry, and therefore the number of MA applications for radiopharmaceuticals is concise. However, the development of innovative radiopharmaceuticals usually takes place in radiopharmacies, research centres or nuclear medicine laboratories. Practically all recent major clinical breakthroughs in Nuclear Medicine over the last decade, exemplified by the success of theranostics with Somatostatin analogs and prostate cancer applications, were based on the use of in-house preparations of these innovative products. In case a new radiopharmaceutical has both the technical (half-life) and clinical potential to be produced and distributed commercially, these new radiopharmaceuticals more frequently make their way to pharmaceutical companies that take over from academia and provide funding for further clinical trials besides phase 0 / phase I. European legislation treats radiopharmaceuticals used in the preparation process of a radiopharmaceutical different than other, i.e., non-radioactive pharmaceuti

Published
2022

28. Cyclotrons operated for Nuclear Medicine and Radiopharmacy in the German speaking D-A-CH countries: An update on current status and trends

Author

Zippel, C., Ermert, J., Patt, M., Gildehaus, F. J., Ross, T. L., Reischl, G., Neumaier, B., (0000-0001-7431-0026) Kiß, O., Mitterhauser, M., Wadsak, W., Schibli, R., (0000-0003-4846-1271) Kopka, K., Zippel, C., Ermert, J., Patt, M., Gildehaus, F. J., Ross, T. L., Reischl, G., Neumaier, B., (0000-0001-7431-0026) Kiß, O., Mitterhauser, M., Wadsak, W., Schibli, R., and (0000-0003-4846-1271) Kopka, K.

Abstract

Background: Cyclotrons form a central infrastructure and are a resource of medical radionu- clides for the development of new radiotracers as well as the production and supply of clini- cally established radiopharmaceuticals for patient care in nuclear medicine. Aim: To provide an updated overview of the number and characteristics of cyclotrons that are currently in use within radiopharmaceutical sciences and for the development of radiopharma- ceuticals to be used for patient care in Nuclear Medicine in Germany (D), Austria (A) and Switzerland (CH). Methods: Publicly available information on the cyclotron infrastructure was (i) consolidated and updated, (ii) supplemented by selective desktop research and, last but not least, (iii) vali- dated by members of the committee of the academic “Working Group Radiochemistry and Radiopharmacy” (AGRR), consisting of radiochemists and radiopharmacists of the D-A-CH countries and belonging to the German Society of Nuclear Medicine (DGN), as well as the Radiopharmaceuticals Committee of the DGN. Results: In total, 39 cyclotrons were identified that are currently being operated for medical radionuclide production for imaging and therapy in Nuclear Medicine clinics, 29 of them in Germany, 4 in Austria and 6 in Switzerland. The majority of the cyclotrons reported (69%) are operated by universities, university hospitals or research institutions close to a university (clinic), less by/in cooperation with industrial partners (26%) or a (non-university) clinic/PET-center (5%). Most of the cyclotrons (82%) are running with up to 18 MeV proton beams, which is sufficient for the production of the currently most common cyclotron-based radionuclides for PET imaging. Discussion: The data presented provide an academically-updated overview of the medical cy- clotrons operated for the production of radiopharmaceuticals and their use in Nuclear Medi- cine in the D-A-CH countries. In this context, we discuss current developments and trends with a

Published
2022

33. Multicenter F-18-PI-2620 PET for in vivo staging of tau pathology in progressive supranuclear palsy

Author

Rullmann, M., additional, Brendel, M., additional, Schroeter, M.L., additional, Saur, D., additional, Rumpf, J.J., additional, Levin, J., additional, Perneczky, R., additional, Tiepolt, S., additional, Patt, M., additional, Mueller, A., additional, Villemagne, V.L., additional, Classen, J., additional, Stephens, A.W., additional, Kovacs, G.G., additional, Sabri, O., additional, and Barthel, H., additional

Published
2022
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34. Serotonin transporter (5-HTT) availability in the dorsal raphe nucleus – a potential biomarker predicting treatment success in highly obese patients

Author

Griebsch, N.I., additional, Kern, J., additional, Kirchmann, J., additional, Rullmann, M., additional, Luthardt, J., additional, Becker, G.A., additional, Patt, M., additional, Meyer, P.M., additional, Hilbert, A., additional, Blüher, M., additional, Dietrich, A., additional, Sabri, O., additional, and Hesse, S., additional

Published
2022
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37. Interplay of tau and functional network connectivity in progressive supranuclear palsy: a [18F]PI-2620 PET/MRI study.

Author

Aghakhanyan, Gayane, Rullmann, M., Rumpf, J., Schroeter, M. L., Scherlach, C., Patt, M., Brendel, M., Koglin, N., Stephens, A. W., Classen, J., Hoffmann, K. T., Sabri, O., and Barthel, H.

Subjects
PROGRESSIVE supranuclear palsy, TAU proteins, BRAIN function localization, MAGNETIC resonance imaging of the brain, TAUOPATHIES
Abstract

Purpose: Progressive supranuclear palsy (PSP) is primary 4-repeat tauopathy. Evidence spanning from imaging studies indicate aberrant connectivity in PSPs. Our goal was to assess functional connectivity network alterations in PSP patients and the potential link between regional tau-burden and network-level functional connectivity using the next-generation tau PET tracer [18F]PI-2620 and resting-state functional MRI (fMRI). Material and methods: Twenty-four probable PSP patients (70.9 ± 6.9 years, 13 female), including 14 Richardson syndrome (RS) and 10 non-RS phenotypes, underwent [18F]PI-2620 PET/MRI imaging. Distribution volume ratios (DVRs) were estimated using non-invasive pharmacokinetic modeling. Resting-state fMRI was also acquired in these patients as well as in thirteen older non-AD MCI reference group (64 ± 9 years, 4 female). The functional network was constructed using 141 by 141 region-to-region functional connectivity metrics (RRC) and network-based statistic was carried out (connection threshold p < 0.001, cluster threshold pFDR < 0.05). Results: In total, 9870 functional connections were analyzed. PSPs compared to aged non-AD MCI reference group expressed aberrant connectivity evidenced by the significant NBS network consisting of 89 ROIs and 118 connections among them (NBS mass 4226, pFDR < 0.05). Tau load in the right globus pallidus externus (GPe) and left dentate nucleus (DN) showed significant effects on functional network connectivity. The network linked with increased tau load in the right GPe was associated with hyperconnectivity of low-range intra-opercular connections (NBS mass 356, pFDR < 0.05), while the network linked with increased tau load in the left cerebellar DN was associated with cerebellar hyperconnectivity and cortico-cerebellar hypoconnectivity (NBS mass 517, pFDR < 0.05). Conclusions: PSP patients show altered functional connectivity. Network incorporating deep gray matter structures demonstrate hypoconnectivity, cerebellum hyperconnectivity, while cortico-cortical connections show variable changes. Tau load in the right GPe and left DN is associated with functional networks which strengthen low-scale intra-opercular and intra-cerebellar connections and weaken opercular-cerebellar connections. These findings support the concept of tau load-dependent functional network changes in PSP, by that providing evidence for downstream effects of neuropathology on brain functionality in this primary tauopathy. [ABSTRACT FROM AUTHOR]

Published
2022
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41. (+)-[18F]Flubatine as a novel α4β2 nicotinic acetylcholine receptor PET ligand – Results of the first-in-human brain imaging application in patients with β-amyloid PET-confirmed Alzheimer’s disease and healthy controls

Author

Tiepolt, S., Becker, G.-A., Wilke, S., Cecchin, D., Rullmann, M., Meyer, P. M., Barthel, H., Hesse, S., Patt, M., Luthardt, J., Wagenknecht, G., Sattler, B., Deuther-Conrad, W., Ludwig, F.-A., Fischer, S., Gertz, H.-J., Smits, R., Hoepping, A., Steinbach, J., Brust, P., and Sabri, O.

Subjects
(+)-[18F]Flubatine, PET, α4β2 nicotinic acetylcholine receptors, kinetic modeling, human brain, (+)-[18F]NCFHEB
Abstract

The cerebral cholinergic system is involved in several cognitive processes and neuropsychiatric 2 diseases. For research purposes and later on in routine clinical settings new PET radioligands with more favorable characteristics than the established 3-pyridylether derivatives with their slow kinetics are necessary. Here we present the first in-human brain PET imaging data of the new α4β2 nicotinic acetylcholine receptor (nAChR)-targeting radioligand (+)-[18F]Flubatine. Primary aim of this study was to develop a kinetic modeling-based approach to quantify the α4β2 nAChR availability in the human brain and to compare respective data of healthy controls (HCs) with those of patients with Alzheimer’s disease (AD). Secondary aims were to investigate whether (+)-[18F]Flubatine binding was correlated to cognitive test data or β-amyloid radiotracer accumulation. Furthermore, the partial volume effect (PVE) on regional (+)-[18F]Flubatine binding was investigated. We examined 11 non-smoking HCs and 9 non-smoking patients with mild AD without anti-dementive drugs. Prior to (+)-[18F]Flubatine PET, all subjects underwent an extensive neuropsychological testing and a β-amyloid [11C]PiB PET/MRI examination. To evaluate the (+)-[18F]Flubatine PET data, we used full kinetic modeling (one and two tissue compartment 16 modeling (1TCM and 2TCM)) and regional as well as voxel-based analyses. 270 min p.i., the unchanged parent compound in arterial blood amounted to 97±2%. As revealed by regional analysis, (+)-[18F]Flubatine distribution volume (binding) was significantly reduced in the bilateral mesial temporal cortex in AD patients compared to HCs (right: AD: 10.6±1.1 vs HC: 11.6±1.4, p=0.049; left: AD: 11.0±1.1 vs HCs:12.2±1.8, p=0.046). Voxel-based analysis detected further clusters of reduced (+)-[18F]Flubatine in left precuneus/posterior cingulate cortex, right superior temporal and left middle temporal cortex (k>30, p0.5, p

Published
2021

42. Sigma-1 and dopamine D2/D3 receptor occupancy of pridopidine in healthy volunteers and patients with Huntington disease: a [18F] fluspidine and [18F] fallypride PET study

Author

Grachev, I. D., Meyer, P. M., Becker, G. A., Bronzel, M., Marsteller, D., Pastino, G., Voges, O., Rabinovich, L., Knebel, H., Zientek, F., Rullmann, M., Sattler, B., Patt, M., Gerhards, T., Strauss, M., Kluge, A., Brust, P., Savola, J.-M., Gordon, M. F., Geva, M., Hesse, S., Barthel, H., Hayden, M. R., and Sabri, O.

Subjects
Sigma-1 receptor occupancy, PETPridopidine, Dopamine D2/D3 receptor occupancy, Huntington disease, [18F]fluspidine
Abstract

Purpose: Pridopidine is an investigational drug for Huntington disease (HD). Pridopidine was originally thought to act as a dopamine stabilizer. However, pridopidine shows highest affinity to the sigma-1 receptor (S1R) and enhances neuroprotection via the S1R in preclinical studies. Using [18F] fluspidine and [18F] fallypride PET, the purpose of this study was to assess in vivo target engagement/receptor occupancy of pridopidine to the S1R and dopamine D2/D3 receptor (D2/D3R) at clinical relevant doses in healthy volunteers (HVs) and as proof-of-concept in a small number of patients with HD. Methods: Using [18F] fluspidine PET (300 MBq, 0–90 min), 11 male HVs (pridopidine 0.5 to 90 mg; six dose groups) and three male patients with HD (pridopidine 90 mg) were investigated twice, without and 2 h after single dose of pridopidine. Using [18F] fallypride PET (200 MBq, 0–210 min), four male HVs were studied without and 2 h following pridopidine administration (90 mg). Receptor occupancy was analyzed by the Lassen plot. Results: S1R occupancy as function of pridopidine dose (or plasma concentration) in HVs could be described by a three-parameter Hill equation with a Hill coefficient larger than one. A high degree of S1R occupancy (87% to 91%) was found throughout the brain at pridopidine doses ranging from 22.5 to 90 mg. S1R occupancy was 43% at 1 mg pridopidine. In contrast, at 90 mg pridopidine, the D2/D3R occupancy was only minimal (~ 3%). Conclusions: Our PET findings indicate that at clinically relevant single dose of 90 mg, pridopidine acts as a selective S1R ligand showing near to complete S1R occupancy with negligible occupancy of the D2/D3R. The dose S1R occupancy relationship suggests cooperative binding of pridopidine to the S1R. Our findings provide significant clarification about pridopidine’s mechanism of action and support further use of the 45-mg twice-daily dose to achieve full and selective targeting of the S1R in future clinical trials of neurodegenerative disorders. Clinical Trials.gov Identifier: NCT03019289 January 12, 2017; EUDRA-CT-Nr. 2016-001757-41. © 2020, The Author(s).

Published
2021

43. Quantification of cerebral nicotinic α7 acetylcholine receptors (α7 nAChRs) under gastric stimulation of the vagus nerve in piglets

Author

Rullmann, M., Alexander Becker, G., Antonov, A., Sattler, B., Sattler, T., Deuther-Conrad, W., Schimpf, S., Patt, M., Meyer, P. M., Teodoro, R., Wenzel, B., Scheunemann, M., Hesse, S., Brust, P., Leitzke, M., and Sabri, O.

Abstract

Introduction Electrical gastric vagus nerve stimulation (VNS) shifts the sympathetic-vagal balance toward a parasympathetic predominance (1). We aim to assess central changes in α7 nAChR-mediated transmission and hypothesize that VNS changes the parasympathetic tone by changing the α7 nAChR availability in the nucleus tractus solitarii (NTS) and distinct cortical and subcortical regions (2). Material and Methods Following a standard 35-frames, 120-min protocol for dynamic brain PET imaging, data from eight piglets (15.6 ± 3.2 kg, ~6 weeks) were acquired post injection of 194.8 ± 9.4 MBq of [18F]DBT-10 (3) followed by T1-MPRAGE MRI: three baseline, two with infusion of the acetylcholine esterase inhibitor physostigmine (0.04 mg/kg, 1 ml/min, at 10 min prior to tracer injection; 0.24 mg/kg, 1 ml/min, at tracer injection/scan start over 120 min) and three with VNS in repeated sequences of 0.5 Hz over 5 min, 5 min pause started at scan start. TACs were analyzed using a 2-tissue compartment model involving a metabolite-corrected arterial input function to generate individual total distribution volumes (VT) as receptor parameter. Results Compared to baseline, we observed an increase of the mean VT after physostigmine infusion (61 %) as well as after VNS (28 %) without major alterations of K1 in the NTS (Figure 1 and 2). Conclusion These initial data indicate blood-flow-independent changes under VNS as compared with baseline suggesting an increase in α7 nAChR availability although the changes appear more heterogeneous in VNS as compared with physostigmine. The finding is in contrast to our hypothesis expecting lower α7 nAChR-availability as a result of increased acetylcholine release following VNS. We speculate that higher VT under VNS may reflect an increase in affinity of the α7 nAChR or result in an upregulation of the α7 nAChR. Increase of VT following physostigmine administration could be related to a positive allosteric effect on the α7 nAChR. Furthermore, the results of this study allow sample size estimations for further preclinical and clinical studies.

Published
2021

44. Feasibility of short imaging protocols for [18F]PI-2620 tau‐PET in progressive supranuclear palsy

Author

Song, M, Scheifele, M, Barthel, H, van Eimeren, T, Beyer, L, Marek, K, Eckenweber, F, Palleis, C, Finze, A, Kaiser, L, Kern, M, Nitschmann, A, Biechele, G, Katzdobler, S, Bischof, GN, Hammes, J, Jessen, F, Saur, D, Schroeter, ML, Rumpf, J, Rullmann, M, Schildan, A, Patt, M, Neumaier, B, Stephens, AW, Rauchmann, B, Perneczky, R, Levin, J, Classen, J, Höglinger, G, Bartenstein, P, Boening, G, Ziegler, S, Villemagne, VLL, Drzezga, A, Seibyl, JP, Sabri, O, Brendel, M, Song, M, Scheifele, M, Barthel, H, van Eimeren, T, Beyer, L, Marek, K, Eckenweber, F, Palleis, C, Finze, A, Kaiser, L, Kern, M, Nitschmann, A, Biechele, G, Katzdobler, S, Bischof, GN, Hammes, J, Jessen, F, Saur, D, Schroeter, ML, Rumpf, J, Rullmann, M, Schildan, A, Patt, M, Neumaier, B, Stephens, AW, Rauchmann, B, Perneczky, R, Levin, J, Classen, J, Höglinger, G, Bartenstein, P, Boening, G, Ziegler, S, Villemagne, VLL, Drzezga, A, Seibyl, JP, Sabri, O, and Brendel, M

Abstract

Background Dynamic 60‐minute positron‐emission‐tomography (PET) imaging with the novel tau radiotracer [18F]PI‐2620 facilitated accurate discrimination between patients with progressive supranuclear palsy (PSP) and healthy controls (HCs). We now aimed to investigate if shorter acquisition and static time windows of [18F]PI‐2620 tau‐PET can be used for imaging of patients with PSP. Method We evaluated 37 patients at five different centers with probable or possible PSP Richardson syndrome (PSP‐RS) together with ten HCs. [18F]PI‐2620 PET was performed by a dynamic 60 minute scan. Distribution volume ratios (DVRs, multilinear reference tissue model 2, cerebellar reference) were calculated using full and truncated scan durations (0‐60, 0‐50, 0‐40, 0‐30, and 0‐20 minutes p.i.). Standardized uptake value ratios (SUVrs, cerebellar reference) were obtained from static imaging windows with 20 minutes duration (20‐40, 30‐50, and 40‐60 minutes p.i.). All DVR and SUVr data were compared with regard to their potential to discriminate patients with PSP‐RS from HCs in predefined subcortical and cortical target regions (effect size, receiver operating area under the curve (AUC), multi‐region classifier). Finally, we tested if shorter [18F]PI‐2620 PET imaging can also be applied to patients with Alzheimer’s disease (n=11). Result The effect size of 0‐50 and 0‐40 DVR was equivalent to 0‐60 DVR (averaged Cohen’s d: 1.22 and 1.16 vs. 1.26), whereas the performance dropped for 0‐30 or 0‐20 DVR. The 20‐40 SUVr indicated the best performance of all short static acquisition windows (averaged Cohen’s d: 0.99). The globus pallidus internus discriminated patients with PSP and healthy controls at a similarly high level for 0‐60 DVR (AUC: 0.96), 0‐40 DVR (AUC: 0.96), and 20‐40 SUVr (AUC: 0.94). The multi‐region classifier sensitivity of these time windows was consistently 86%. 0‐40 DVR showed similar performance in Alzheimer’s disease when compared to 0‐60 DVR. Conclusion Short dynamic acquisiti

Published
2021

45. Guideline on current good radiopharmacy practice (cGRPP) for the small-scale preparation of radiopharmaceuticals

Author

Gillings, N., Hjelstuen, O., Ballinger, J., Behe, M., Decristoforo, C., Elsinga, P., Ferrari, V., Peitl, P.K., Koziorowski, J., Laverman, P., Mindt, T.L., Neels, O., Ocak, M., Patt, M., Todde, S., Gillings, N., Hjelstuen, O., Ballinger, J., Behe, M., Decristoforo, C., Elsinga, P., Ferrari, V., Peitl, P.K., Koziorowski, J., Laverman, P., Mindt, T.L., Neels, O., Ocak, M., Patt, M., and Todde, S.

Abstract

Contains fulltext : 232903.pdf (Publisher’s version ) (Open Access), This guideline on current good radiopharmacy practice (cGRPP) for small-scale preparation of radiopharmaceuticals represents the view of the Radiopharmacy Committee of the European Association of Nuclear Medicine (EANM). The guideline is laid out in the format of the EU Good Manufacturing Practice (GMP) guidelines as defined in EudraLex volume 4. It is intended for non-commercial sites such as hospital radiopharmacies, nuclear medicine departments, research PET centres and in general any healthcare establishments. In the first section, general aspects which are applicable to all levels of operations are discussed. The second section discusses the preparation of small-scale radiopharmaceuticals (SSRP) using licensed generators and kits. Finally, the third section goes into the more complex preparation of SSRP from non-licensed starting materials, often requiring a purification step and sterile filtration. The intention is that the guideline will assist radiopharmacies in the preparation of diagnostic and therapeutic SSRP's safe for human administration.

Published
2021

46. Binding characteristics of [18F]PI-2620 distinguish the clinically predicted tau isoform in different tauopathies by PET

Author

Song, M, Beyer, L, Kaiser, L, Barthel, H, van Eimeren, T, Marek, K, Nitschmann, A, Scheifele, M, Palleis, C, Respondek, G, Kern, M, Biechele, G, Hammes, J, Bischof, G, Barbe, M, Onur, O, Jessen, F, Saur, D, Schroeter, ML, Rumpf, J-J, Rullmann, M, Schildan, A, Patt, M, Neumaier, B, Barret, O, Madonia, J, Russell, DS, Stephens, AW, Mueller, A, Roeber, S, Herms, J, Botzel, K, Danek, A, Levin, J, Classen, J, Hoglinger, GU, Bartenstein, P, Villemagne, V, Drzezga, A, Seibyl, J, Sabri, O, Boening, G, Ziegler, S, Brendel, M, Song, M, Beyer, L, Kaiser, L, Barthel, H, van Eimeren, T, Marek, K, Nitschmann, A, Scheifele, M, Palleis, C, Respondek, G, Kern, M, Biechele, G, Hammes, J, Bischof, G, Barbe, M, Onur, O, Jessen, F, Saur, D, Schroeter, ML, Rumpf, J-J, Rullmann, M, Schildan, A, Patt, M, Neumaier, B, Barret, O, Madonia, J, Russell, DS, Stephens, AW, Mueller, A, Roeber, S, Herms, J, Botzel, K, Danek, A, Levin, J, Classen, J, Hoglinger, GU, Bartenstein, P, Villemagne, V, Drzezga, A, Seibyl, J, Sabri, O, Boening, G, Ziegler, S, and Brendel, M

Abstract

The novel tau-PET tracer [18F]PI-2620 detects the 3/4-repeat-(R)-tauopathy Alzheimer's disease (AD) and the 4R-tauopathies corticobasal syndrome (CBS) and progressive supranuclear palsy (PSP). We determined whether [18F]PI-2620 binding characteristics deriving from non-invasive reference tissue modelling differentiate 3/4R- and 4R-tauopathies. Ten patients with a 3/4R tauopathy (AD continuum) and 29 patients with a 4R tauopathy (CBS, PSP) were evaluated. [18F]PI-2620 PET scans were acquired 0-60 min p.i. and the distribution volume ratio (DVR) was calculated. [18F]PI-2620-positive clusters (DVR ≥ 2.5 SD vs. 11 healthy controls) were evaluated by non-invasive kinetic modelling. R1 (delivery), k2 & k2a (efflux), DVR, 30-60 min standardized-uptake-value-ratios (SUVR30-60) and the linear slope of post-perfusion phase SUVR (9-60 min p.i.) were compared between 3/4R- and 4R-tauopathies. Cortical clusters of 4R-tau cases indicated higher delivery (R1SRTM: 0.92 ± 0.21 vs. 0.83 ± 0.10, p = 0.0007), higher efflux (k2SRTM: 0.17/min ±0.21/min vs. 0.06/min ± 0.07/min, p < 0.0001), lower DVR (1.1 ± 0.1 vs. 1.4 ± 0.2, p < 0.0001), lower SUVR30-60 (1.3 ± 0.2 vs. 1.8 ± 0.3, p < 0.0001) and flatter slopes of the post-perfusion phase (slope9-60: 0.006/min ± 0.007/min vs. 0.016/min ± 0.008/min, p < 0.0001) when compared to 3/4R-tau cases. [18F]PI-2620 binding characteristics in cortical regions differentiate 3/4R- and 4R-tauopathies. Higher tracer clearance indicates less stable binding in 4R tauopathies when compared to 3/4R-tauopathies.

Published
2021

47. Aktuelle radiopharmazeutische Entwicklungen für die theranostische Anwendung

Author

(0000-0001-7431-0026) Neels, O., Kratochwil, C., Patt, M., (0000-0001-7431-0026) Neels, O., Kratochwil, C., and Patt, M.

Abstract

Im vorliegenden CME-Beitrag sollen die Grundlagen des Theranostik-Prinzips beginnend bei den Eigenschaften der Radionuklide sowie deren Verfügbarkeit erläutert werden. Anhand von medizinischen und chemischen Beispielen aus den prominentesten Anwendungsgebieten der Theranostik (Prostatakarzinom/PSMA, neuroendokrine Tumoren und Fibroblasten-Aktivierungsprotein Inhibitoren) werden die unterschiedlichen Arten von theranostischen Radionuklid- und Radioliganden-Paaren beschrieben. Abgerundet wird der Artikel durch Ausführungen zu den regulatorischen Randbedingungen wie Verfügbarkeit und Verkehrsfähigkeit von Radionuklidvorstufen und radioaktiven Arzneimitteln sowie zu deren Eigenherstellung.

Published
2021

48. Sigma-1 and dopamine D2/D3 receptor occupancy of pridopidine in healthy volunteers and patients with Huntington disease: a [18F] fluspidine and [18F] fallypride PET study

Author

Grachev, I., Meyer, P., Becker, G., Bronzel, M., Marsteller, D., Pastino, G., Voges, O., Rabinovich, L., Knebel, H., Zientek, F., Rullmann, M., Sattler, B., Patt, M., Gerhards, T., Strauss, M., Kluge, A., (0000-0001-5555-7058) Brust, P., Savola, J., Gordon, M., Geva, M., Hesse, S., Barthel, H., Hayden, M., Sabri, O., Grachev, I., Meyer, P., Becker, G., Bronzel, M., Marsteller, D., Pastino, G., Voges, O., Rabinovich, L., Knebel, H., Zientek, F., Rullmann, M., Sattler, B., Patt, M., Gerhards, T., Strauss, M., Kluge, A., (0000-0001-5555-7058) Brust, P., Savola, J., Gordon, M., Geva, M., Hesse, S., Barthel, H., Hayden, M., and Sabri, O.

Abstract

Pridopidine is an investigational drug in late stage development for the treatment of Huntington disease and originally postulated to act as dopamine stabilizer by modulating dopamine-dependent motor behavior. However, preclinical studies show pridopidine has highest affinity to sigma-1 receptors. Importantly, mediated by sigma-1 receptors, pridopidine has neuroprotective properties and enhances neuronal plasticity. The aim of our study was to determine the in-vivo the target engagement (receptor occupancy) of pridopidine at clinically relevant doses in healthy volunteers and Huntington disease patients. We used sigma-1 receptor-specific (S)-(-)-[18F]Fluspidine and dopamine D2/D3 receptor-specific [18F]Fallypride PET imaging to quantify the sigma-1 and dopamine D2/D3 receptor occupancy of pridopidine. Eleven male healthy volunteers (pridopidine 0.5 to 90 mg in six dose groups) and three male Huntington disease patients (pridopidine 90 mg) were studied twice before and 2h following single oral doses of pridopidine using S-(-)-[18F]Fluspidine PET (300 MBq, 0-90min p.i.). Distribution volume VT was quantified using kinetic modeling (One-tissue compartment model; metabolite correction). Four male healthy volunteers were studied twice using [18F]Fallpride PET (200 MBq, 0-210min p.i.) before and 2h after a single oral dose of pridopidine (90 mg). Binding potential BPND was assessed by the simplified reference model. Volume-of-interest analyses were performed. For each subject/tracer, the receptor occupancy was calculated by the Lassen plot analysis. In healthy volunteers, there was high sigma-1 receptor occupancy (87 to 91%) across all brain regions at doses ranging from 22.5 to 90 mg. The sigma-1 receptor occupancy was 43% at 1 mg pridopidine. In Huntington disease patients, very similar to healthy volunteers, at 90 mg pridopidine, there was high sigma-1 receptor occupancy (87±7%, n.s.). In contrast, in healthy volunteers, there was only negligible dopamine D2/D3 recepto

Published
2021

49. Emerging radionuclides in a regulatory framework for medicinal products – how do they fit?

Author

Decristoforo, C., (0000-0001-7431-0026) Neels, O., Patt, M., Decristoforo, C., (0000-0001-7431-0026) Neels, O., and Patt, M.

Abstract

Recent years have seen the establishment of several radionuclides as medicinal products in particular in the setting of theranostics and PET. [177Lu]Lutetium Chloride or [64Cu]Copper Chloride have received marketing authorization as radionuclide precursor [68Ga]Gallium Chloride has received regulatory approval in the form of different 68Ge/68Ga generators. This is a formal requirement by the EU directive 2001/83, even though for some of these radionuclide precursors no licensed kit is available that can be combined to obtain a final radiopharmaceuticals, as it is the case for Technetium-99m. In view of several highly promising, especially metallic radionuclides for theranostic applications in a wider sense, the strict regulatory environment poses the risk of slowing down development, in particular for radionuclide producers that want to provide innovative radionuclide for clinical research purposes, which is the basis for their further establishment. In this position paper we address the regulatory framework for novel radionuclides within the EU, the current challenges in particular related to clinical translation and potential options to support translational development within Europe and worldwide.

Published
2021

50. Highlight selection of radiochemistry and radiopharmacy developments by editorial board

Author

Aime, S., Al-Qahtani, M., Behe, M., Bormans, G., Carlucci, G., Dasilva, J., Decristoforo, C., Duatti, A., Elsinga, P., (0000-0003-4846-1271) Kopka, K., Li, X., Liu, Z., Mach, R., Middel, O., Passchier, J., Patt, M., Penuelas, I., Rey, A., Scott, P., Todde, S., Toyohara, J., Vugts, D., Yang, Z., Aime, S., Al-Qahtani, M., Behe, M., Bormans, G., Carlucci, G., Dasilva, J., Decristoforo, C., Duatti, A., Elsinga, P., (0000-0003-4846-1271) Kopka, K., Li, X., Liu, Z., Mach, R., Middel, O., Passchier, J., Patt, M., Penuelas, I., Rey, A., Scott, P., Todde, S., Toyohara, J., Vugts, D., and Yang, Z.

Abstract

Background: The Editorial Board of EJNMMI Radiopharmacy and Chemistry releases a biyearly highlight commentary to update the readership on trends in the field of radiopharmaceutical development. Results: This commentary of highlights has resulted in 23 different topics selected by each member of the Editorial Board addressing a variety of aspects ranging from novel radiochemistry to first in man application of novel radiopharmaceuticals. Conclusion: Trends in radiochemistry and radiopharmacy are highlighted demonstrating the progress in the research field being the scope of EJNMMI Radiopharmacy and Chemistry.

Published
2021

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