123I-iododexetimide preferentially binds to the muscarinic receptor subtype M1 in vivo

Geor Bakker; Wilhelmina A Vingerhoets; Jan-Peter van Wieringen; Kora de Bruin; Jos Eersels; Jan de Jong; Youssef Chahid; Bart P Rutten; Susan DuBois; Megan Watson; Adrian J Mogg; Hongling Xiao; Michael Crabtree; David A Collier; Christian C Felder; Vanessa N Barth; Lisa M Broad; Oswald J Bloemen; Thérèse A van Amelsvoort; Jan Booij

doi:10.2967/jnumed.114.147488

123I-iododexetimide preferentially binds to the muscarinic receptor subtype M1 in vivo

Geor Bakker, Wilhelmina A Vingerhoets, Jan-Peter van Wieringen, Kora de Bruin, Jos Eersels, Jan de Jong, Youssef Chahid, Bart P Rutten, Susan DuBois, Megan Watson, Adrian J Mogg, Hongling Xiao, Michael Crabtree, David A Collier, Christian C Felder, Vanessa N Barth, Lisa M Broad, Oswald J Bloemen, Thérèse A van Amelsvoort, Jan Booij

Supporting clinical sciences

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15 Citations (Scopus)

Abstract

UNLABELLED: The muscarinic M1 receptor (M1R) is highly involved in cognition, and selective M1 agonists have procognitive properties. Loss of M1R has been found in postmortem brain tissue for several neuropsychiatric disorders and may be related to symptoms of cognitive dysfunction. (123)I-iododexetimide is used for imaging muscarinic acetylcholine receptors (mAchRs). Considering its high brain uptake and intense binding in M1R-rich brain areas, (123)I-iododexetimide may be an attractive radiopharmaceutical to image M1R. To date, the binding affinity and selectivity of (123)I-iododexetimide for the mAchR subtypes has not been characterized, nor has its brain distribution been studied intensively. Therefore, this study aimed to address these topics.

METHODS: The in vitro affinity and selectivity of (127)I-iododexetimide (cold-labeled iododexetimide), as well as its functional antagonist properties (guanosine 5'-[γ-(35)S-thio]triphosphate [GTPγ(35)S] assay), were assessed on recombinant human M1R-M5R. Distributions of (127)I-iododexetimide and (123)I-iododexetimide in the brain were evaluated using liquid chromatography-mass spectrometry and storage phosphor imaging, respectively, ex vivo in rats, wild-type mice, and M1-M5 knock-out (KO) mice. Inhibition of (127)I-iododexetimide and (123)I-iododexetimide binding in M1R-rich brain areas by the M1R/M4R agonist xanomeline, or the antipsychotics olanzapine (M1R antagonist) and haloperidol (low M1R affinity), was assessed in rats ex vivo.

RESULTS: In vitro, (127)I-iododexetimide displayed high affinity for M1R (pM range), with modest selectivity over other mAchRs. In biodistribution studies on rats, ex vivo (127)I-iododexetimide binding was much higher in M1R-rich brain areas, such as the cortex and striatum, than in cerebellum (devoid of M1Rs). In M1 KO mice, but not M2-M5 KO mice, (127)I-iododexetimide binding was strongly reduced in the frontal cortex compared with wild-type mice. Finally, acute administration of both an M1R/M4R agonist xanomeline and the M1R antagonist olanzapine was able to inhibit (123)I-iododexetimide ex vivo, and (123)I-iododexetimide binding in M1-rich brain areas in rats, whereas administration of haloperidol had no effect.

CONCLUSION: The current results suggest that (123)I-iododexetimide preferentially binds to M1R in vivo and can be displaced by M1R ligands. (123)I-iododexetimide may therefore be a useful imaging tool as a way to further evaluate M1R changes in neuropsychiatric disorders, as a potential stratifying biomarker, or as a clinical target engagement biomarker to assess M1R.

Original language	English
Pages (from-to)	317-322
Number of pages	6
Journal	Journal of Nuclear Medicine
Volume	56
Issue number	2
DOIs	https://doi.org/10.2967/jnumed.114.147488
Publication status	Published - Feb 2015

Keywords

Animals
Binding, Competitive
Biomarkers
Chromatography, Liquid
Cognition
Dexetimide
Humans
Iodine Radioisotopes
Ligands
Male
Protein Binding
Rats
Rats, Sprague-Dawley
Receptor, Muscarinic M1
Receptors, Muscarinic
Recombinant Proteins
Tandem Mass Spectrometry
Tissue Distribution
Tomography, Emission-Computed, Single-Photon
Journal Article
Research Support, Non-U.S. Gov't

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10.2967/jnumed.114.147488

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Bakker, G., Vingerhoets, W. A., van Wieringen, J-P., de Bruin, K., Eersels, J., de Jong, J., Chahid, Y., Rutten, B. P., DuBois, S., Watson, M., Mogg, A. J., Xiao, H., Crabtree, M., Collier, D. A., Felder, C. C., Barth, V. N., Broad, L. M., Bloemen, O. J., van Amelsvoort, T. A., & Booij, J. (2015). 123I-iododexetimide preferentially binds to the muscarinic receptor subtype M1 in vivo. Journal of Nuclear Medicine, 56(2), 317-322. https://doi.org/10.2967/jnumed.114.147488

Bakker, Geor ; Vingerhoets, Wilhelmina A ; van Wieringen, Jan-Peter ; de Bruin, Kora ; Eersels, Jos ; de Jong, Jan ; Chahid, Youssef ; Rutten, Bart P ; DuBois, Susan ; Watson, Megan ; Mogg, Adrian J ; Xiao, Hongling ; Crabtree, Michael ; Collier, David A ; Felder, Christian C ; Barth, Vanessa N ; Broad, Lisa M ; Bloemen, Oswald J ; van Amelsvoort, Thérèse A ; Booij, Jan. / 123I-iododexetimide preferentially binds to the muscarinic receptor subtype M1 in vivo. In: Journal of Nuclear Medicine. 2015 ; Vol. 56, No. 2. pp. 317-322.

@article{6e724601be754b15bcd262dfa6e70bf8,

title = "123I-iododexetimide preferentially binds to the muscarinic receptor subtype M1 in vivo",

abstract = "UNLABELLED: The muscarinic M1 receptor (M1R) is highly involved in cognition, and selective M1 agonists have procognitive properties. Loss of M1R has been found in postmortem brain tissue for several neuropsychiatric disorders and may be related to symptoms of cognitive dysfunction. (123)I-iododexetimide is used for imaging muscarinic acetylcholine receptors (mAchRs). Considering its high brain uptake and intense binding in M1R-rich brain areas, (123)I-iododexetimide may be an attractive radiopharmaceutical to image M1R. To date, the binding affinity and selectivity of (123)I-iododexetimide for the mAchR subtypes has not been characterized, nor has its brain distribution been studied intensively. Therefore, this study aimed to address these topics.METHODS: The in vitro affinity and selectivity of (127)I-iododexetimide (cold-labeled iododexetimide), as well as its functional antagonist properties (guanosine 5'-[γ-(35)S-thio]triphosphate [GTPγ(35)S] assay), were assessed on recombinant human M1R-M5R. Distributions of (127)I-iododexetimide and (123)I-iododexetimide in the brain were evaluated using liquid chromatography-mass spectrometry and storage phosphor imaging, respectively, ex vivo in rats, wild-type mice, and M1-M5 knock-out (KO) mice. Inhibition of (127)I-iododexetimide and (123)I-iododexetimide binding in M1R-rich brain areas by the M1R/M4R agonist xanomeline, or the antipsychotics olanzapine (M1R antagonist) and haloperidol (low M1R affinity), was assessed in rats ex vivo.RESULTS: In vitro, (127)I-iododexetimide displayed high affinity for M1R (pM range), with modest selectivity over other mAchRs. In biodistribution studies on rats, ex vivo (127)I-iododexetimide binding was much higher in M1R-rich brain areas, such as the cortex and striatum, than in cerebellum (devoid of M1Rs). In M1 KO mice, but not M2-M5 KO mice, (127)I-iododexetimide binding was strongly reduced in the frontal cortex compared with wild-type mice. Finally, acute administration of both an M1R/M4R agonist xanomeline and the M1R antagonist olanzapine was able to inhibit (123)I-iododexetimide ex vivo, and (123)I-iododexetimide binding in M1-rich brain areas in rats, whereas administration of haloperidol had no effect.CONCLUSION: The current results suggest that (123)I-iododexetimide preferentially binds to M1R in vivo and can be displaced by M1R ligands. (123)I-iododexetimide may therefore be a useful imaging tool as a way to further evaluate M1R changes in neuropsychiatric disorders, as a potential stratifying biomarker, or as a clinical target engagement biomarker to assess M1R.",

keywords = "Animals, Binding, Competitive, Biomarkers, Chromatography, Liquid, Cognition, Dexetimide, Humans, Iodine Radioisotopes, Ligands, Male, Protein Binding, Rats, Rats, Sprague-Dawley, Receptor, Muscarinic M1, Receptors, Muscarinic, Recombinant Proteins, Tandem Mass Spectrometry, Tissue Distribution, Tomography, Emission-Computed, Single-Photon, Journal Article, Research Support, Non-U.S. Gov't",

author = "Geor Bakker and Vingerhoets, {Wilhelmina A} and {van Wieringen}, Jan-Peter and {de Bruin}, Kora and Jos Eersels and {de Jong}, Jan and Youssef Chahid and Rutten, {Bart P} and Susan DuBois and Megan Watson and Mogg, {Adrian J} and Hongling Xiao and Michael Crabtree and Collier, {David A} and Felder, {Christian C} and Barth, {Vanessa N} and Broad, {Lisa M} and Bloemen, {Oswald J} and {van Amelsvoort}, {Th{\'e}r{\`e}se A} and Jan Booij",

note = "{\textcopyright} 2015 by the Society of Nuclear Medicine and Molecular Imaging, Inc.",

year = "2015",

month = feb,

doi = "10.2967/jnumed.114.147488",

language = "English",

volume = "56",

pages = "317--322",

journal = "Journal of Nuclear Medicine",

issn = "0161-5505",

publisher = "Society of Nuclear Medicine Inc.",

number = "2",

}

Bakker, G, Vingerhoets, WA, van Wieringen, J-P, de Bruin, K, Eersels, J, de Jong, J, Chahid, Y, Rutten, BP, DuBois, S, Watson, M, Mogg, AJ, Xiao, H, Crabtree, M, Collier, DA, Felder, CC, Barth, VN, Broad, LM, Bloemen, OJ, van Amelsvoort, TA & Booij, J 2015, '123I-iododexetimide preferentially binds to the muscarinic receptor subtype M1 in vivo', Journal of Nuclear Medicine, vol. 56, no. 2, pp. 317-322. https://doi.org/10.2967/jnumed.114.147488

123I-iododexetimide preferentially binds to the muscarinic receptor subtype M1 in vivo. / Bakker, Geor; Vingerhoets, Wilhelmina A; van Wieringen, Jan-Peter; de Bruin, Kora; Eersels, Jos; de Jong, Jan; Chahid, Youssef; Rutten, Bart P; DuBois, Susan; Watson, Megan; Mogg, Adrian J; Xiao, Hongling; Crabtree, Michael; Collier, David A; Felder, Christian C; Barth, Vanessa N; Broad, Lisa M; Bloemen, Oswald J; van Amelsvoort, Thérèse A; Booij, Jan.

In: Journal of Nuclear Medicine, Vol. 56, No. 2, 02.2015, p. 317-322.

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

TY - JOUR

T1 - 123I-iododexetimide preferentially binds to the muscarinic receptor subtype M1 in vivo

AU - Bakker, Geor

AU - Vingerhoets, Wilhelmina A

AU - van Wieringen, Jan-Peter

AU - de Bruin, Kora

AU - Eersels, Jos

AU - de Jong, Jan

AU - Chahid, Youssef

AU - Rutten, Bart P

AU - DuBois, Susan

AU - Watson, Megan

AU - Mogg, Adrian J

AU - Xiao, Hongling

AU - Crabtree, Michael

AU - Collier, David A

AU - Felder, Christian C

AU - Barth, Vanessa N

AU - Broad, Lisa M

AU - Bloemen, Oswald J

AU - van Amelsvoort, Thérèse A

AU - Booij, Jan

PY - 2015/2

Y1 - 2015/2

N2 - UNLABELLED: The muscarinic M1 receptor (M1R) is highly involved in cognition, and selective M1 agonists have procognitive properties. Loss of M1R has been found in postmortem brain tissue for several neuropsychiatric disorders and may be related to symptoms of cognitive dysfunction. (123)I-iododexetimide is used for imaging muscarinic acetylcholine receptors (mAchRs). Considering its high brain uptake and intense binding in M1R-rich brain areas, (123)I-iododexetimide may be an attractive radiopharmaceutical to image M1R. To date, the binding affinity and selectivity of (123)I-iododexetimide for the mAchR subtypes has not been characterized, nor has its brain distribution been studied intensively. Therefore, this study aimed to address these topics.METHODS: The in vitro affinity and selectivity of (127)I-iododexetimide (cold-labeled iododexetimide), as well as its functional antagonist properties (guanosine 5'-[γ-(35)S-thio]triphosphate [GTPγ(35)S] assay), were assessed on recombinant human M1R-M5R. Distributions of (127)I-iododexetimide and (123)I-iododexetimide in the brain were evaluated using liquid chromatography-mass spectrometry and storage phosphor imaging, respectively, ex vivo in rats, wild-type mice, and M1-M5 knock-out (KO) mice. Inhibition of (127)I-iododexetimide and (123)I-iododexetimide binding in M1R-rich brain areas by the M1R/M4R agonist xanomeline, or the antipsychotics olanzapine (M1R antagonist) and haloperidol (low M1R affinity), was assessed in rats ex vivo.RESULTS: In vitro, (127)I-iododexetimide displayed high affinity for M1R (pM range), with modest selectivity over other mAchRs. In biodistribution studies on rats, ex vivo (127)I-iododexetimide binding was much higher in M1R-rich brain areas, such as the cortex and striatum, than in cerebellum (devoid of M1Rs). In M1 KO mice, but not M2-M5 KO mice, (127)I-iododexetimide binding was strongly reduced in the frontal cortex compared with wild-type mice. Finally, acute administration of both an M1R/M4R agonist xanomeline and the M1R antagonist olanzapine was able to inhibit (123)I-iododexetimide ex vivo, and (123)I-iododexetimide binding in M1-rich brain areas in rats, whereas administration of haloperidol had no effect.CONCLUSION: The current results suggest that (123)I-iododexetimide preferentially binds to M1R in vivo and can be displaced by M1R ligands. (123)I-iododexetimide may therefore be a useful imaging tool as a way to further evaluate M1R changes in neuropsychiatric disorders, as a potential stratifying biomarker, or as a clinical target engagement biomarker to assess M1R.

AB - UNLABELLED: The muscarinic M1 receptor (M1R) is highly involved in cognition, and selective M1 agonists have procognitive properties. Loss of M1R has been found in postmortem brain tissue for several neuropsychiatric disorders and may be related to symptoms of cognitive dysfunction. (123)I-iododexetimide is used for imaging muscarinic acetylcholine receptors (mAchRs). Considering its high brain uptake and intense binding in M1R-rich brain areas, (123)I-iododexetimide may be an attractive radiopharmaceutical to image M1R. To date, the binding affinity and selectivity of (123)I-iododexetimide for the mAchR subtypes has not been characterized, nor has its brain distribution been studied intensively. Therefore, this study aimed to address these topics.METHODS: The in vitro affinity and selectivity of (127)I-iododexetimide (cold-labeled iododexetimide), as well as its functional antagonist properties (guanosine 5'-[γ-(35)S-thio]triphosphate [GTPγ(35)S] assay), were assessed on recombinant human M1R-M5R. Distributions of (127)I-iododexetimide and (123)I-iododexetimide in the brain were evaluated using liquid chromatography-mass spectrometry and storage phosphor imaging, respectively, ex vivo in rats, wild-type mice, and M1-M5 knock-out (KO) mice. Inhibition of (127)I-iododexetimide and (123)I-iododexetimide binding in M1R-rich brain areas by the M1R/M4R agonist xanomeline, or the antipsychotics olanzapine (M1R antagonist) and haloperidol (low M1R affinity), was assessed in rats ex vivo.RESULTS: In vitro, (127)I-iododexetimide displayed high affinity for M1R (pM range), with modest selectivity over other mAchRs. In biodistribution studies on rats, ex vivo (127)I-iododexetimide binding was much higher in M1R-rich brain areas, such as the cortex and striatum, than in cerebellum (devoid of M1Rs). In M1 KO mice, but not M2-M5 KO mice, (127)I-iododexetimide binding was strongly reduced in the frontal cortex compared with wild-type mice. Finally, acute administration of both an M1R/M4R agonist xanomeline and the M1R antagonist olanzapine was able to inhibit (123)I-iododexetimide ex vivo, and (123)I-iododexetimide binding in M1-rich brain areas in rats, whereas administration of haloperidol had no effect.CONCLUSION: The current results suggest that (123)I-iododexetimide preferentially binds to M1R in vivo and can be displaced by M1R ligands. (123)I-iododexetimide may therefore be a useful imaging tool as a way to further evaluate M1R changes in neuropsychiatric disorders, as a potential stratifying biomarker, or as a clinical target engagement biomarker to assess M1R.

KW - Animals

KW - Binding, Competitive

KW - Biomarkers

KW - Chromatography, Liquid

KW - Cognition

KW - Dexetimide

KW - Humans

KW - Iodine Radioisotopes

KW - Ligands

KW - Male

KW - Protein Binding

KW - Rats

KW - Rats, Sprague-Dawley

KW - Receptor, Muscarinic M1

KW - Receptors, Muscarinic

KW - Recombinant Proteins

KW - Tandem Mass Spectrometry

KW - Tissue Distribution

KW - Tomography, Emission-Computed, Single-Photon

KW - Journal Article

KW - Research Support, Non-U.S. Gov't

U2 - 10.2967/jnumed.114.147488

DO - 10.2967/jnumed.114.147488

M3 - Article

C2 - 25593117

VL - 56

SP - 317

EP - 322

JO - Journal of Nuclear Medicine

JF - Journal of Nuclear Medicine

SN - 0161-5505

IS - 2

ER -

123I-iododexetimide preferentially binds to the muscarinic receptor subtype M1 in vivo

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