Trontinemab

Trontinemab
Monoclonal antibody
Type?
Clinical data
Other namesRG6102
Legal status
Legal status
  • Investigational
Identifiers
CAS Number
UNII

Trontinemab (RG6102) is a monoclonal antibody (mAb) developed by Roche/Genentech for the treatment of Alzheimer's disease. It is based on gantenerumab, an anti-amyloid monoclonal antibody, and uses a brainshuttle domain to enhance its permeability through the blood–brain barrier.[1] Compared to gantenerumab, it has 50 times as much penetrance into the brain.[2][3][4][5]

Mechanism of action

Trontinemab consists of the anti-amyloid mAb ganterenumab, fused with a Fab fragment that binds to human transferrin receptor 1 (TfR1) in the Fc domain.[6] The fully-human mAb gantenerumab preferentially targets fibrils and Aβ oligomers over the monomer form (KD: 0.6, 1.2, and 17 nM for the three forms, respectively). After binding to the Aβ, gantenerumab elicits amyloid clearance through microglia-mediated phagocytosis.[1] Gantenerumab showed some amyloid clearance in human trials, especially at high doses; however, its lower-than-expected amyloid removal capacity, its inability to slow the disease progression, even at high doses, and its side effects, including amyloid-related imaging abnormalities (ARIAs), prevent the mAb from entering clinical practice.[7]

To improve safety and efficacy, scientists tried to increase gantenerumab's ability to cross the blood–brain barrier by adding to the mAb a Fab fragment (brainshuttle module) that binds to one of the receptors expressed on the cells that make up the blood–brain barrier. The binding would then trigger endocytosis of the mAb, allowing it to be transported through the cell and released into the brain. Trontinemab contains a single anti-TfR1 Fab fragment bound to the Fc region, because initial testing showed that mAbs with two Fab fragments were easily degraded by lysosomes and had an inferior transportation efficiency compared to mAbs with a single anti-TfR1 Fab.[8] The Fab fragment is strategically inverted to prevent antibody-dependent cellular cytotoxicity toward TfR1-expressing cells. When the brainshuttle module binds to TfR1, the mAb assumes a position that allows the two anti-amyloid arms to clash with each other and with the Fc receptors of the FcγR class on effector cells, preventing these cells from engaging the Fc domain of the mAb.[9] The resulting mAb, trontinemab, has the following characteristics:

  • 50 times greater penetrability potential of the blood–brain barrier relative to the original mAb.[1]
  • Even distribution throughout the brain.[1]
  • Low incidence of ARIAs, possibly due to the mAb entering mostly through small blood vessels—almost skipping entirely the aggregated amyloid-beta plaques on the big vessels.[10]
  • Low immune reaction to TfR1-expressing cells.[9]

Development history

Trontinemab was first developed under the code name RG6102 or, as referred to by Roche/Genentech, brain-shuttle gantenerumab. A phase 1 dose-escalation study in healthy volunteers presented at the Alzheimer's Disease and Parkinson's Disease Conference 2021 showed a half-life of 3 to 6 days and a linear relationship between plasma and cerebrospinal fluid (CSF) concentrations. Brain exposure, measured by CSF/plasma ratio, increased from 0.1% for normal IgG to 0.8% with brain-shuttle gantenerumab.[11] After gantenerumab failed in two phase-III trials, Roche changed the name of "brainshuttle gantenerumab" to trontinemab.[12]

Following the first-in-human study, a phase-Ib/II study, "BrainShuttle AD", was launched. Patients enrolled in the study were randomized to a placebo group or one of the 0.2, 0.6, 1.8, or 3.6 mg/kg cohorts. The drug was initially shown to be effective at the 1.8 mg/kg dose, with amyloid-beta levels dropping by an average of 84 centiloids—centiloid (CL) is a scale that quantifies amyloid-PET activity in the brain measured by tracers like florbetapir (18F)—on day 84. Amyloid-beta concentration dropped below the threshold of amyloid positivity (24.1 CL) in 75% of participants.[13] Further analysis showed that the 3.6 mg/kg cleared an average of 107 CL on day 84.[14] After combining the results of both parts 1 and 2 of the study, the highest dose group cleared a mean of 99 CL. Further, 91% of the participants in the 3.6 mg/kg cohort were below the amyloid-positivity threshold, and amyloid-PET burden was reduced to below 11 CL in 72% of them.[15] In the highest-dose group, there were no non-responders.[16]

Aβ depletion was early, deep, and even, with all lobes of the neocortex showing amyloid burden below 24 CL.[16] Brain regions showing rapid amyloid depletion temporarily shrank due to the large volume of amyloid removed. When amyloid beta had been cleared, the reduction stopped.[17] Trontinemab treatment increased Aβ42 concentration and Aβ42/40 ratio in the CSF, as well as decreased disease biomarkers, including total Tau protein, pTau181, neurogranin, and SNAP25 levels.[16]

As for the safety profile, the most common adverse effects were infusion-related reactions (IRRs) and anemia. The incidence of IRRs lessened when more aggressive premedication with steroids was used, while the incidence of anemia was attributed to frequent blood draws and was considered infrequent and mild. ARIA (both ARIA-E and ARIA-H) was uncommon, with a combined incidence of 4.1% in the highest dose group.[15] There was a fatal case in the 1.8 mg/kg cohort—a 78-year-old woman with hemorrhagic bleeding in her right frontal lobe on day 44. She had been considered a person with a high bleeding risk due to her screening tests showing that she had superficial siderosis and genetic factors, which are the signs of probable cerebral amyloid angiopathy. The trial's protocol was amended after her death to exclude those with superficial siderosis.[14]

At the 2025 Alzheimer's Association International Conference, Roche announced plans for two phase-III, identically designed trials, TRONTIER 1 and TRONTIER 2, both of which are actively[as of?] enrolling patients with mild-to-moderate AD. Participants will go through a master prescreening study called TRAVELLER, then undergo an 8-week screening phase, and be randomized into two cohorts: one receiving trontinemab at 3.6 mg/kg (every 4 weeks for the first 24 weeks, then the dosing interval extends to every 12 weeks), and the other receiving a placebo. The trial includes patients with Mini–Mental State Examination (MMSE) scores of 2.2 or higher and Clinical Dementia Rating scores between 0.5 and 1, aged 50 to 90, with evidence of amyloid pathology. Excluded are individuals with any brain macrohemorrhage, four or more microhemorrhages, severe white matter disease, or other conditions that could impact cognition.[18]

References

  1. ^ a b c d Grimm, Hans Peter; Schumacher, Vanessa; Schäfer, Martin; Imhof-Jung, Sabine; Freskgård, Per-Ola; Brady, Kevin; Hofmann, Carsten; Rüger, Petra; Schlothauer, Tilman; Göpfert, Ulrich; Hartl, Maximilian; Rottach, Sylvia; Zwick, Adrian; Seger, Shanon; Neff, Rachel (2023). "Delivery of the Brainshuttle™ amyloid-beta antibody fusion trontinemab to non-human primate brain and projected efficacious dose regimens in humans". mAbs. 15 (1) 2261509. doi:10.1080/19420862.2023.2261509. ISSN 1942-0870. PMC 10572082. PMID 37823690.
  2. ^ Steenhuysen, Julie (2022-12-01). "Roche shutters most trials of Alzheimer's drug after failed trials". Reuters. Retrieved 2023-11-26.
  3. ^ Zhang, Yun; Chen, Huaqiu; Li, Ran; Sterling, Keenan; Song, Weihong (30 June 2023). "Amyloid β-based therapy for Alzheimer's disease: challenges, successes and future". Signal Transduction and Targeted Therapy. 8 (1): 248. doi:10.1038/s41392-023-01484-7. ISSN 2059-3635. PMC 10310781. PMID 37386015.
  4. ^ Grimm, Hans Peter; Schumacher, Vanessa; Schäfer, Martin; Imhof-Jung, Sabine; Freskgård, Per-Ola; Brady, Kevin; Hofmann, Carsten; Rüger, Petra; Schlothauer, Tilman; Göpfert, Ulrich; Hartl, Maximilian; Rottach, Sylvia; Zwick, Adrian; Seger, Shanon; Neff, Rachel; Niewoehner, Jens; Janssen, Niels (2023). "Delivery of the Brainshuttle™ amyloid-beta antibody fusion trontinemab to non-human primate brain and projected efficacious dose regimens in humans". mAbs. 15 (1) 2261509. doi:10.1080/19420862.2023.2261509. ISSN 1942-0870. PMC 10572082. PMID 37823690.
  5. ^ Kulic, Luka; Vogt, Annamarie; Alcaraz, Fabien; Barrington, Philip; Marchesi, Maddalena; Klein, Gregory; Croney, Ruth; Agnew, David; Abrantes, João A.; Svoboda, Hanno (1 September 2022). "053 Brainshuttle AD: Investigating safety, tolerability, and PK/PD of RG6102 in prodromal/mild-to-moderate AD". Journal of Neurology, Neurosurgery & Psychiatry. 93 (9): e2. doi:10.1136/jnnp-2022-abn2.97. ISSN 0022-3050. S2CID 251518048.
  6. ^ "Trontinemab". AlzForum. 31 August 2025. Retrieved 31 August 2025.
  7. ^ "[Ad hoc announcement pursuant to Art. 53 LR] Roche provides update on Phase III GRADUATE programme evaluating gantenerumab in early Alzheimer's disease". Roche (Press release). 14 November 2022. Retrieved 31 August 2025.
  8. ^ Niewoehner, Jens; Bohrmann, Bernd; Collin, Ludovic; Urich, Eduard; Sade, Hadassah; Maier, Peter; Rueger, Petra; Stracke, Jan Olaf; Lau, Wilma; Tissot, Alain C.; Loetscher, Hansruedi; Ghosh, Anirvan; Freskgård, Per-Ola (2014-01-08). "Increased Brain Penetration and Potency of a Therapeutic Antibody Using a Monovalent Molecular Shuttle". Neuron. 81 (1): 49–60. doi:10.1016/j.neuron.2013.10.061. ISSN 0896-6273. PMID 24411731.
  9. ^ a b Weber, Felix; Bohrmann, Bernd; Niewoehner, Jens; Fischer, Jens A. A.; Rueger, Petra; Tiefenthaler, Georg; Moelleken, Joerg; Bujotzek, Alexander; Brady, Kevin; Singer, Thomas; Ebeling, Martin; Iglesias, Antonio; Freskgård, Per-Ola (2018-01-02). "Brain Shuttle Antibody for Alzheimer's Disease with Attenuated Peripheral Effector Function due to an Inverted Binding Mode". Cell Reports. 22 (1): 149–162. doi:10.1016/j.celrep.2017.12.019. ISSN 2211-1247. PMID 29298417.
  10. ^ Mummery, Catherine (27 July 2025). "A four-part Featured Research Session including expert presentations on the development of new drug delivery methods in Alzheimer's disease, the latest results from the Phase Ia/IIb Brainshuttle™ AD study, and the future of the trontinemab clinical development program: Next wave of innovation in Alzheimer's disease therapeutics: The value of novel active transport mechanisms". medically.roche.com (Presentation slides). p. 10. Retrieved 31 August 2025.
  11. ^ Kulic, Luka (10 March 2021). "Translation of RG6102, an amyloid-targeting therapy with superior brain penetration properties, to the clinic". medically.roche.com (Presentation slides). p. 13. Retrieved 31 August 2025.
  12. ^ Armstrong, Annalee (1 December 2022). "Roche thins Alzheimer's program after phase 3 failure, may seek 'external partnerships'". Fierce Pharma. Retrieved 31 August 2025.
  13. ^ Kulic, Luka (25 October 2023). "THE ANTI-AMYLOID BETA "BRAIN SHUTTLE" ANTIBODY TRONTINEMAB RAPIDLY REDUCES AMYLOID PLAQUES IN PARTICIPANTS WITH ALZHEIMER'S DISEASE". medically.roche.com (Presentation slides). p. 15. Retrieved 1 September 2025.
  14. ^ a b Kulic, Luka; Alcaraz, Fabien; Klein, Gregory; Hofmann, Carsten; Yilmaz, Stella; Abrantes, João A.; Sickert, Denise; Marchesi, Maddalena; Wojtowicz, Jakub; Croney, Ruth; Agnew, David; Ahlers, Silke; Delmar, Paul; Svoboda, Hanno; Wiesel, Iris (30 October 2024). "LATEST INTERIM RESULTS FROM THE BRAINSHUTTLE AD STUDY, A PHASE IB/IIA STUDY OF TRONTINEMAB IN PEOPLE WITH ALZHEIMER'S DISEASE". medically.roche.com (Presentation slides). Retrieved 31 August 2025.
  15. ^ a b Kulic, Luka (27 July 2025). "A four-part Featured Research Session including expert presentations on the development of new drug delivery methods in Alzheimer's disease, the latest results from the Phase Ia/IIb Brainshuttle™ AD study, and the future of the trontinemab clinical development program: Latest results from the dose-expansion part (Part 2) of the Brainshuttle™AD study of trontinemab in people with Alzheimer's disease". medically.roche.com (Presentation slides). pp. 28, 30. Retrieved 1 September 2025.
  16. ^ a b c Klein, Gregory (27 July 2025). "A four-part Featured Research Session including expert presentations on the development of new drug delivery methods in Alzheimer's disease, the latest results from the Phase Ia/IIb Brainshuttle™ AD study, and the future of the trontinemab clinical development program: Interim biomarker results for trontinemab, a novel Brainshuttle™ antibody in development for the treatment of Alzheimer's disease". medically.roche.com (Presentation slides). pp. 46, 48, 51, 52, 53. Retrieved 1 September 2025.
  17. ^ Klein, Gregory (3 April 2025). "Interim biomarker results of trontinemab, a novel Brainshuttle TM antibody in development for the treatment of Alzheimer's disease". medically.roche.com (Presentation slides). Retrieved 1 September 2025.
  18. ^ Smith, Janice (27 July 2025). "TRONTIER 1 and TRONTIER 2: Pivotal trials of trontinemab in early symptomatic Alzheimer's disease". medically.roche.com (Presentation slides). Retrieved 1 September 2025.

Content Disclaimer

Informasi ini disarikan dari Wikipedia dan disajikan kembali untuk tujuan edukasi. Konten tersedia di bawah lisensi CC BY-SA 3.0. Kami tidak bertanggung jawab atas ketidakakuratan data yang bersumber dari kontribusi publik tersebut.

  1. The information displayed on this website is sourced in part or in whole from Wikipedia and has been adapted for the purpose of restating it. We strive to provide accurate and relevant information, however:
  2. There is no guarantee of absolute accuracy. Wikipedia is an open, collaborative project that can be edited by anyone, so information is subject to change.
  3. It is not intended to constitute professional advice. The content displayed is for informational and educational purposes only. For important decisions (e.g., medical, legal, or financial), please consult a professional.
  4. Content copyright. Wikipedia is licensed under the Creative Commons Attribution-ShareAlike License (CC BY-SA). This means that content may be reused with appropriate attribution and shared under a similar license.
  5. Responsible use. Any risk arising from the use of information from this website is entirely the responsibility of the user.