Overview
Name: SAR228810
Therapy Type: Immunotherapy (passive) (timeline)
Target Type: Amyloid-Related (timeline)
Condition(s): Alzheimer's Disease
U.S. FDA Status: Alzheimer's Disease (Discontinued)
Company: Sanofi
Background
This is a monoclonal antibody directed primarily against soluble protofibrillar and fibrillar species of Aβ. It is relatively inactive against Aβ monomers and small oligomeric aggregates. This humanized antibody was engineered on an IgG4 backbone. Its parent murine mAb, SAR255952, is reported to have low effector function, which is thought to reduce the risk of amyloid-related imaging abnormalities (ARIA). SAR228810 reportedly has low binding affinity for activating FcγRs on human microglia and no binding to complement C1q, a pro-inflammatory component of the innate immune system. The rationale is that these features confer less risk of a proinflammatory response leading to vasogenic edema and cerebral microhemorrhage. In APPSL transgenic mice, the antibody prevented amyloid accumulation, microglia activation, and synaptic dysfunction, without causing vascular changes (Pradier et al., 2018).
Findings
From 2012-2015, a multicenter Phase 1 trial tested six ascending doses of intravenous infusion and two doses of subcutaneous injection on safety, pharmacokinetics, and pharmacodynamic endpoints in 48 patients at sites in Sweden and other countries.
Sanofi stopped development of SAR228810 in late 2018, citing pipeline prioritization as the reason (see slide 29 of 2018 year-end results presentation).
For trial details, see clinicaltrials.gov
Last Updated: 28 Jul 2021
Further Reading
No Available Further Reading
Overview
Name: Octagam®10%
Synonyms: Intravenous Immunoglobulin, NewGam
Therapy Type: Immunotherapy (passive) (timeline)
Target Type: Amyloid-Related (timeline), Inflammation (timeline)
Condition(s): Alzheimer's Disease, Mild Cognitive Impairment
U.S. FDA Status: Alzheimer's Disease (Inactive), Mild Cognitive Impairment (Inactive)
Company: Octapharma
Approved for: Immunodeficiency disorders
Background
NewGam/Octagam® is an intravenous immunoglobulin preparation by the Switzerland-based company Octapharma. It is a marketed product. The rationale of evaluating it in Alzheimer's disease, as for other intravenous immunoglobulin preparations such as Gammagard® and Flebogamma (as Gamunex), is that naturally occurring polyclonal autoantibodies against Aβ may be protective and are reduced in Alzheimer's disease (see Weksler et al., 2002).
Findings
The first trial of this IVIG preparation in Alzheimer's evaluated six different doses of Octagam 10 percent against two placebo comparators in a six-month trial of 58 people with mild to moderate AD. This multicenter Phase 2 trial has been completed. This trial missed its primary endpoint of change in plasma Aβ levels, and was negative for most of its secondary biomarker outcomes with the exception of a signal suggesting a benefit for cerebral metabolism. None of the doses tested showed any benefit for cognition or function (see Dodel et al, 2013; Feb 2013 news).
A second, single-center Phase 2 study conducted at Sutter Institute for Medical Research in Sacramento, California, investigated the long-term effects of a short course of this IVIG preparation. Octagam 10 percent (0.4 g/kg) or saline placebo was infused every other week for two months in 50 people with amnestic MCI due to AD, with two years of follow-up. Initial results on 28 patients assessed one year after treatment indicated possible effects on the Clinical Dementia Rating Sum of Boxes and brain atrophy as seen on MRI (see Mar 2013 conference story). Full publication of the data reported less brain atrophy and a treatment benefit on ADAS-cog13 and MMSE in the IVIG group compared to the placebo group at 12 months; these differences disappeared by 24 months. The paper also reported a trend toward fewer progressions to AD dementia in the treated group at 12 months, and argued for additional research on this approach (Kile et al., 2015). In additional follow up of 27 participants, treatment did not change brain volume, cognition, or conversion to dementia at five years (Kile et al., 2021).
A single center, proof of mechanism study in five people with MCI due to AD measured brain amyloid by florbetapir PET and retinal amyloid by autofluorescent imaging. All received five infusions of 0.4 g/kg Octagam 10 percent over two months. In three of the five participants, brain amyloid was reduced one month after the last infusion; all five had lowering of amyloid in at least one eye (Kile et al., 2020).
A metanalysis of five clinical trials of intravenous immunoglobulin formulations found no evidence for improved cognition or disease modification in people with Alzheimer’s disease or MCI (Liu and Wang, 2019).
Clinical Trial Timeline
- Phase 2
- Study completed / Planned end date
- Planned end date unavailable
- Study aborted
| Sponsor |
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| Octapharma |
NCT00812565 |
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| Sutter Health |
NCT01300728 |
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Last Updated: 17 Sep 2021
Further Reading
No Available Further Reading
Submitted by elizabethwu1 on 
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