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Background

There is very little reported human experience with cell therapy for AD. We test the safety of using Wnt‐activated adipose tissue‐derived stem cells (ADSCs) injected directly into the ventricles of the brain to address multifactorial etiologies.

Method

Two million and 5 million expanded, Wnt‐expressing, ADSCs were tested in the first 5 patients ("low‐dose and medium‐dose") of a Phase 1 FDA clinical trial using escalating doses. Participants had age <80 years, FAST stages 4 and 5, and cognitive, amyloid PET centiloid scores, and CSF analyses consistent with AD. The participants underwent: 1) lipoaspiration and cell preparation, 2) Ommaya reservoir implantation, and 3) infusion of a single dose of the test product via Ommaya reservoir. The primary endpoint was safety. Secondary endpoints included normalization of phosphorylated tau (p ‐Tau), and amyloid beta, and improvement in cognitive testing scores.

Result

Adverse events (AEs) from pre‐injection surgical procedures included mild bruising and discomfort. Test product injection showed no AEs (range: 23‐55 weeks) including headache or nausea (Figure 1). At 12 weeks post‐injection, CSF phosphorylated tau (p ‐Tau) improved in 80% of the participants from a median of 60.2 pg/ml (range: 46.9 ‐ 76.1) to a normal median of 36.8 (range 15.0 – 66.6), amyloid PET scan centiloid scores decreased in 60% of participants from a pre‐injection median of 137.2 (range: 55.33 – 155.47) to a median of 100.53 (range: 55.58 – 168.1, Figure 3). ADAS‐cog scores improved in 80% of participants by week 12 from a pre‐injection median of 53 (range: 40 – 69) to a median of 38 (range: 20 – 69, Figure 4), MMSE scores improved in 60% of participants by week 12 from a pre‐injection median of 16 (range: 14 – 19) to a median of 18 (range: 12 – 20).

Conclusion

This "first‐in‐human" trial of intracerebroventricular injection of expanded autologous, Wnt‐expressing, adipose tissue‐derived stem cells proved well‐tolerated and safe for the low‐dose and medium dose cohorts. Secondary endpoints showed promising improvements.

Details

1009240
Subject
Stem cells;
Nausea;
Alzheimer's disease;
Body fat;
Contusions;
Brain;
Safety;
Clinical trials;
Clinical research;
Cognition;
Mini-Mental State Examination;
Humans;
Neuroimaging;
Discomfort;
Critical incidents;
Patients;
Tests;
Normalization;
Dosage
Title
Early results of a "First‐in‐Human" Phase 1 clinical study of intracerebroventricular injections of ex vivo expanded, autologous, Wnt‐activated, adipose‐derived stem cells in participants with mild to moderate Alzheimer's Disease (AD)
Author
Duma, Christopher M. 1 ; Keirstead, Hans 1 ; Nistor, Gabriel 1 ; Lynn, Robert 1 ; Buxton, Jessica J. 2 ; Hareng, Zoe M 3 ; Chung, Karlyssa 1 ; Alva, Gustavo 4 ; Farmer, Sawyer H. 5 ; Harris, Ashley 6 

 Regeneration Biomedical, Inc., Newport Beach, CA, USA 
 University of California, Berkeley, Berkeley, CA, USA 
 Regeneration Biomedical, Inc., NEWPORT BEACH, CA, USA 
 ATP Clinical Research, Costa Mesa, CA, USA 
 Albany Medical College, Albany, NY, USA 
 Brain and Spine Surgeons of Orange County, Newport Beach, CA, USA 
Publication title
Alzheimer's & Dementia; Chicago
Volume
21
Supplement
S7
Number of pages
4
Publication year
2025
Publication date
Dec 1, 2025
Section
DRUG DEVELOPMENT
Publisher
John Wiley & Sons, Inc.
Place of publication
Chicago
Country of publication
United States
Publication subject
Gerontology And Geriatrics, Medical Sciences--Psychiatry And Neurology
ISSN
1552-5260
e-ISSN
1552-5279
Source type
Scholarly Journal
Language of publication
English
Document type
Journal Article
Publication history
 
 
Online publication date
2025-12-23
Milestone dates
2025-12-23 (publishedOnlineFinalForm)
Publication history
 
 
   First posting date
23 Dec 2025
DOI
https://doi.org/10.1002/alz70861_108493
ProQuest document ID
3286013154
Document URL
https://www.proquest.com/scholarly-journals/early-results-first-human-phase-1-clinical-study/docview/3286013154/se-2?accountid=208611
Copyright
© 2025. This work is published under http://creativecommons.org/licenses/by/4.0/ (the "License"). Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License.
Last updated
2026-01-02
Database
ProQuest One Academic