Clinical evaluation of [18F] JNJ-64326067, a novel candidate PET tracer for the detection of tau pathology in Alzheimer’s disease

Purpose The accumulation of misfolded tau is a common feature of several neurodegenerative disorders, with Alzheimer’s disease (AD) being the most common. Earlier we identified JNJ-64326067, a novel isoquinoline derivative with high affinity and selectivity for tau aggregates from human AD brain. We...

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Published in	European journal of nuclear medicine and molecular imaging Vol. 47; no. 13; pp. 3176 - 3185
Main Authors	Schmidt, Mark E., Janssens, Luc, Moechars, Diederik, Rombouts, Frederik J. R., Timmers, Maarten, Barret, Olivier, Constantinescu, Cristian C., Madonia, Jennifer, Russell, David S., Sandiego, Christine M., Kolb, Hartmuth
Format	Journal Article
Language	English
Published	Berlin/Heidelberg Springer Berlin Heidelberg 01.12.2020 Springer Nature B.V
Subjects	Adolescent Aggregates Alzheimer Disease - diagnostic imaging Alzheimer's disease Amyloid Aniline Compounds Brain Brain - diagnostic imaging Brain - metabolism Cardiology Cerebellum Computed tomography Cortex (parietal) Digital video recorders Disease control Dosimeters Dosimetry Female Fluorine isotopes Fluorine Radioisotopes Humans Imaging Isoquinolines Kinetics Male Medicine Medicine & Public Health Neurodegenerative diseases Neurology Nuclear Medicine Occipital lobe Oncology Original Original Article Orthopedics Positron emission Positron emission tomography Pyridines Quantitation Radiology Radiopharmaceuticals Selectivity Tau protein tau Proteins - metabolism Temporal cortex Tomography Isoquinoline Alzheimer’s disease Tau aggregates PET
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Abstract	Purpose The accumulation of misfolded tau is a common feature of several neurodegenerative disorders, with Alzheimer’s disease (AD) being the most common. Earlier we identified JNJ-64326067, a novel isoquinoline derivative with high affinity and selectivity for tau aggregates from human AD brain. We report the dosimetry of [ 18 F] JNJ-64326067 and results of a proof-of-concept study comparing subjects with probable Alzheimer’s disease to age-matched healthy controls. Methods [ 18 F] JNJ-64326067 PET scans were acquired for 90 min and then from 120 to 180 min in 5 participants with [ 18 F]-florbetapir PET amyloid positive probable AD (73 ± 9 years) and 5 [ 18 F]-florbetapir PET amyloid negative healthy controls (71 ± 7 years). Whole-body [ 18 F] JNJ-64326067 PET CT scans were acquired in six healthy subjects for 5.5 h in 3 scanning sessions. Brain PET scans were visually reviewed. Regional quantification included kinetic analysis of distribution volume ration (DVR) estimated by Logan graphical analysis over the entire scan and static analysis of SUVr in late frames. Both methods used ventral cerebellar cortex as a reference region. Results One of the healthy controls had focal areas of PET signal in occipital and parietal cortex underlying the site of a gunshot injury as an adolescent; the other four healthy subjects had no tau brain signal. Four of the 5 AD participants had visually apparent retention of [ 18 F] JNJ-64326067 in relevant cortical regions. One of the AD subjects was visually negative. Cortical signal in visually positive subjects approached steady state by 120 min. Temporal and frontal cortical SUVr/DVR values in visually positive AD subjects ranged from 1.21 to 3.09/1.2 to 2.18 and from 0.92 to 1.28/0.91 to 1.16 in healthy controls. Whole-body effective dose was estimated to be 0.0257 mSv/MBq for females and 0.0254 mSv/MBq for males. Conclusions [ 18 F] JNJ-64326067 could be useful for detection and quantitation of tau aggregates.
AbstractList	PurposeThe accumulation of misfolded tau is a common feature of several neurodegenerative disorders, with Alzheimer’s disease (AD) being the most common. Earlier we identified JNJ-64326067, a novel isoquinoline derivative with high affinity and selectivity for tau aggregates from human AD brain. We report the dosimetry of [18F] JNJ-64326067 and results of a proof-of-concept study comparing subjects with probable Alzheimer’s disease to age-matched healthy controls.Methods[18F] JNJ-64326067 PET scans were acquired for 90 min and then from 120 to 180 min in 5 participants with [18F]-florbetapir PET amyloid positive probable AD (73 ± 9 years) and 5 [18F]-florbetapir PET amyloid negative healthy controls (71 ± 7 years). Whole-body [18F] JNJ-64326067 PET CT scans were acquired in six healthy subjects for 5.5 h in 3 scanning sessions. Brain PET scans were visually reviewed. Regional quantification included kinetic analysis of distribution volume ration (DVR) estimated by Logan graphical analysis over the entire scan and static analysis of SUVr in late frames. Both methods used ventral cerebellar cortex as a reference region.ResultsOne of the healthy controls had focal areas of PET signal in occipital and parietal cortex underlying the site of a gunshot injury as an adolescent; the other four healthy subjects had no tau brain signal. Four of the 5 AD participants had visually apparent retention of [18F] JNJ-64326067 in relevant cortical regions. One of the AD subjects was visually negative. Cortical signal in visually positive subjects approached steady state by 120 min. Temporal and frontal cortical SUVr/DVR values in visually positive AD subjects ranged from 1.21 to 3.09/1.2 to 2.18 and from 0.92 to 1.28/0.91 to 1.16 in healthy controls. Whole-body effective dose was estimated to be 0.0257 mSv/MBq for females and 0.0254 mSv/MBq for males.Conclusions[18F] JNJ-64326067 could be useful for detection and quantitation of tau aggregates. Purpose The accumulation of misfolded tau is a common feature of several neurodegenerative disorders, with Alzheimer’s disease (AD) being the most common. Earlier we identified JNJ-64326067, a novel isoquinoline derivative with high affinity and selectivity for tau aggregates from human AD brain. We report the dosimetry of [ 18 F] JNJ-64326067 and results of a proof-of-concept study comparing subjects with probable Alzheimer’s disease to age-matched healthy controls. Methods [ 18 F] JNJ-64326067 PET scans were acquired for 90 min and then from 120 to 180 min in 5 participants with [ 18 F]-florbetapir PET amyloid positive probable AD (73 ± 9 years) and 5 [ 18 F]-florbetapir PET amyloid negative healthy controls (71 ± 7 years). Whole-body [ 18 F] JNJ-64326067 PET CT scans were acquired in six healthy subjects for 5.5 h in 3 scanning sessions. Brain PET scans were visually reviewed. Regional quantification included kinetic analysis of distribution volume ration (DVR) estimated by Logan graphical analysis over the entire scan and static analysis of SUVr in late frames. Both methods used ventral cerebellar cortex as a reference region. Results One of the healthy controls had focal areas of PET signal in occipital and parietal cortex underlying the site of a gunshot injury as an adolescent; the other four healthy subjects had no tau brain signal. Four of the 5 AD participants had visually apparent retention of [ 18 F] JNJ-64326067 in relevant cortical regions. One of the AD subjects was visually negative. Cortical signal in visually positive subjects approached steady state by 120 min. Temporal and frontal cortical SUVr/DVR values in visually positive AD subjects ranged from 1.21 to 3.09/1.2 to 2.18 and from 0.92 to 1.28/0.91 to 1.16 in healthy controls. Whole-body effective dose was estimated to be 0.0257 mSv/MBq for females and 0.0254 mSv/MBq for males. Conclusions [ 18 F] JNJ-64326067 could be useful for detection and quantitation of tau aggregates. The accumulation of misfolded tau is a common feature of several neurodegenerative disorders, with Alzheimer's disease (AD) being the most common. Earlier we identified JNJ-64326067, a novel isoquinoline derivative with high affinity and selectivity for tau aggregates from human AD brain. We report the dosimetry of [ F] JNJ-64326067 and results of a proof-of-concept study comparing subjects with probable Alzheimer's disease to age-matched healthy controls. [ F] JNJ-64326067 PET scans were acquired for 90 min and then from 120 to 180 min in 5 participants with [ F]-florbetapir PET amyloid positive probable AD (73 ± 9 years) and 5 [ F]-florbetapir PET amyloid negative healthy controls (71 ± 7 years). Whole-body [ F] JNJ-64326067 PET CT scans were acquired in six healthy subjects for 5.5 h in 3 scanning sessions. Brain PET scans were visually reviewed. Regional quantification included kinetic analysis of distribution volume ration (DVR) estimated by Logan graphical analysis over the entire scan and static analysis of SUVr in late frames. Both methods used ventral cerebellar cortex as a reference region. One of the healthy controls had focal areas of PET signal in occipital and parietal cortex underlying the site of a gunshot injury as an adolescent; the other four healthy subjects had no tau brain signal. Four of the 5 AD participants had visually apparent retention of [ F] JNJ-64326067 in relevant cortical regions. One of the AD subjects was visually negative. Cortical signal in visually positive subjects approached steady state by 120 min. Temporal and frontal cortical SUVr/DVR values in visually positive AD subjects ranged from 1.21 to 3.09/1.2 to 2.18 and from 0.92 to 1.28/0.91 to 1.16 in healthy controls. Whole-body effective dose was estimated to be 0.0257 mSv/MBq for females and 0.0254 mSv/MBq for males. [ F] JNJ-64326067 could be useful for detection and quantitation of tau aggregates.
Author	Kolb, Hartmuth Russell, David S. Rombouts, Frederik J. R. Timmers, Maarten Barret, Olivier Constantinescu, Cristian C. Schmidt, Mark E. Madonia, Jennifer Sandiego, Christine M. Moechars, Diederik Janssens, Luc
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Keywords	Isoquinoline Alzheimer’s disease Tau aggregates PET
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Snippet	Purpose The accumulation of misfolded tau is a common feature of several neurodegenerative disorders, with Alzheimer’s disease (AD) being the most common.... The accumulation of misfolded tau is a common feature of several neurodegenerative disorders, with Alzheimer's disease (AD) being the most common. Earlier we... PurposeThe accumulation of misfolded tau is a common feature of several neurodegenerative disorders, with Alzheimer’s disease (AD) being the most common....
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SubjectTerms	Adolescent Aggregates Alzheimer Disease - diagnostic imaging Alzheimer's disease Amyloid Aniline Compounds Brain Brain - diagnostic imaging Brain - metabolism Cardiology Cerebellum Computed tomography Cortex (parietal) Digital video recorders Disease control Dosimeters Dosimetry Female Fluorine isotopes Fluorine Radioisotopes Humans Imaging Isoquinolines Kinetics Male Medicine Medicine & Public Health Neurodegenerative diseases Neurology Nuclear Medicine Occipital lobe Oncology Original Original Article Orthopedics Positron emission Positron emission tomography Pyridines Quantitation Radiology Radiopharmaceuticals Selectivity Tau protein tau Proteins - metabolism Temporal cortex Tomography
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Title	Clinical evaluation of [18F] JNJ-64326067, a novel candidate PET tracer for the detection of tau pathology in Alzheimer’s disease
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