Developing canine hepatocyte culture systems is critical for liver transplantation, toxicity evaluation, and drug metabolism studies. However, maintaining viable and functional hepatocytes in long-term cultures remains challenging. Our prior research demonstrated differentiation of cryopreserved canine hepatocytes into hepatic progenitor cells (cHPCs) using three small-molecule compounds: Y-27632 (ROCK inhibitor), A-83-01 (TGFβ inhibitor), and CHIR99021 (GSK3 inhibitor). Nevertheless, rematuration into functional hepatocytes was not achieved. This study aimed to evaluate the differentiation of progenitor cells into mature hepatocytes, compare two-dimensional (2D) and three-dimensional (3D) culture systems, and determine the advantages of 3D culture.

Methods:

cHPCs were cultured in 2D cultures with HGF and oncostatin M or in 3D cultures using AggreWell400^TM plates to form spheroids, transferred to low-adherent plates, and cultured with shaking. Cells were analyzed for morphology, gene expression, and protein markers using immunocytochemistry.

Results:

In 2D cultures, rematuration produced cells with wider cytoplasm, multiple nuclei, and a paving stone-like morphology. Spheroids in 3D cultures reached 150 μm in diameter with irregular edges by day 5. Quantitative real-time polymerase chain reaction analysis revealed significant upregulation of liver-specific genes. In 2D cultures, KRT19 expression increased 1.7-fold compared with cHPCs(p < 0.01). In 3D cultures, ALB (63-fold), TAT (9-fold), MRP2 (34-fold), EpCAM (1.6-fold), CYP2E1 (10-fold), and CYP3A12 (56-fold) were all significantly upregulated compared with cHPCs (p < 0.05). Immunohistochemistry showed robust AFP, ALB, and CYP2E1 expression in 3D cultures, with 87.6 % of cells AFP-positive and 100 % CYP2E1-positive compared to 11.4 % and 7.9 % in 2D cultures, respectively.

Conclusions:

3D rocking culture markedly enhanced liver-specific gene and protein expression, producing functional liver spheroids. These findings underscore the potential of 3D rocking cultures to create reliable, in vivo-like liver models for research and therapeutic applications.

01 Dec 2025·Regenerative Therapy

Transplantation of chemically induced liver progenitors in Nagase analbuminemic rats under liver regenerative stimulus

Article

Author: Eguchi, Susumu ; Imamura, Hajime ; Soyama, Akihiko ; Adachi, Tomohiko ; Yamashita, Mampei ; Fukumoto, Masayuki ; Matsushima, Hajime ; Miyamoto, Daisuke ; Kanetaka, Kengo ; Hara, Takanobu

Methods:

Male Sprague Dawley rats were used for mature hepatocytes (HEP) isolation to induce CLiP using 3 small molecules cocktail (ROCK-inhibitor, TGF beta-1 inhibitor, GSK3 inhibitor). Harvested rat CLiP (1 × 10⁶) were transplanted to the posterior lobe of the liver (30 % of whole liver) of Nagase analbuminemic rats (NAR) through portal vein injection. One week later, portal venous branch to non-transplanted lobe was ligated to induce liver regeneration in CLiP bearing liver lobe (portal branch ligation: PBL). Only CLiP Tx or HEP Tx of same dose were used as control groups. Serial measurement of serum albumin level was measured by ELISA method. All NARs were subject to immunosuppression therapy using tacrolimus s.q. 3 days per week.

Results:

After HEP Tx especially with PBL, serum albumin level was significantly elevated. However, even with PBL, CLiP Tx group did not show significant increase in serum albumin. CLiP were surrounded by tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) positive cells in portal veins suggesting that CLiP were exposed to the risk of innate immunity.

Conclusion:

Although CLiP respond to growth factors and proliferate better than HEP in vitro, their behavior in vivo in response to liver regenerative stimulus were not similar to in vitro probably because of less immaturity of receptors and/or high immunogenicity as compared to HEP.

01 Nov 2025·BIOORGANIC CHEMISTRY

Advances in targeting glycogen synthase kinase 3β for diabetes therapy

Review

Author: Zhong, Ling ; Wang, Fuyu ; Xiao, Wenjing ; Shi, Jianyou ; Bai, Lan ; Li, Yating

Diabetes mellitus is a chronic metabolic disease characterized by hyperglycemia, which is caused by absolute or relative insulin deficiency in secretion and impaired insulin utilization. The newly added content is as follows: Diabetes mellitus is typically classified into two main types: type 1 diabetes (T1DM) and type 2 diabetes (T2DM). Type 1 diabetes primarily arises from the erroneous attack on pancreatic β-cells by the autoimmune system, resulting in β-cell damage and an absolute deficiency in insulin secretion. Genetic factors play a crucial role in its pathogenesis. In contrast, the pathogenesis of type 2 diabetes is more complex, mainly involving insulin resistance and relative insulin deficiency. Its onset is closely linked to both genetic factors and lifestyle, with high-calorie diets, insufficient physical activity, and obesity being significant risk factors.Despite the differences in their pathogenic mechanisms, insulin plays an extremely important role in both types of diabetes. Glycogen synthase kinase 3 (GSK3) is a highly conserved kinase that can activate glycogen synthase. As a key molecule in the glucose metabolic pathway, GSK3β is involved in various cellular activities and plays a crucial role in multiple diseases. Therefore, pharmacological inhibition of the activity and expression of GSK3β represents a promising approach for the treatment of diabetes. In recent years, GSK3 has been implicated in skeletal muscle insulin resistance in obese animal models and obese individuals with type 2 diabetes mellitus (T2DM). It leads to increased glucose production and decreased insulin sensitivity by inhibiting glycogen synthase. These findings indicate that studies utilizing specific and sensitive GSK3 inhibitors have provided new insights into the role of GSK3 in regulating the effect of insulin on glucose transport in muscles. However, diabetes therapeutic drugs targeting GSK3β directly have not yet been approved for marketing worldwide. Herein, we describe the role of GSK3β in diabetes, clarify the central role of GSK3β in cellular signaling pathways, and summarize GSK3β inhibitors for the treatment of diabetes. Finally, we hope that these latest research advances will facilitate the discovery of safe and effective GSK3β inhibitors for the treatment of diabetes.

News (Medical) associated with [11C]OCM-44

30 Apr 2024

·www.sciencedaily.com

Researchers target neurogenesis in new approach to treat Parkinson's disease

Researchers have found a way to better control the preclinical generation of key neurons depleted in Parkinson's disease, pointing toward a new approach for a disease with no cure and few effective treatments. Researchers at the University of Toronto have found a way to better control the preclinical generation of key neurons depleted in Parkinson's disease, pointing toward a new approach for a disease with no cure and few effective treatments. The researchers used an antibody to selectively activate a receptor in a molecular signaling pathway to develop dopaminergic neurons. These neurons produce dopamine, a neurotransmitter critical to brain health. Researchers around the world have been working to coax stem cells to differentiate into dopaminergic neurons, to replace those lost in patients living with Parkinson's disease. But efforts have been hindered in part by an inability to target specific receptors and areas of the brain. "We used synthetic antibodies that we had previously developed to target the Wnt signaling pathway," said Stephane Angers, principal investigator on the study and director of the Donnelly Centre for Cellular and Molecular Biology. "We can selectively activate this pathway to direct stem cells in the midbrain to develop into neurons by targeting specific receptors in the pathway," said Angers, who is also a professor in the Leslie Dan Faculty of Pharmacy and the Temerty Faculty of Medicine, and holds the Charles H. Best Chair of Medical Research at U of T. "This activation method has not been explored before." The study was recently published in the journal Development. Parkinson's disease is the second-most common neurological disorder after Alzheimer's, affecting over 100,000 Canadians. It particularly impacts older men, progressively impairing movement and causing pain as well as sleep and mental health issues. Most previous research efforts to activate the Wnt signaling pathway have relied on a GSK3 enzyme inhibitor. This method involves multiple signaling pathways for stem cell proliferation and differentiation, which can lead to unintended effects on the newly produced neurons and activation of off-target cells. "We developed an efficient method for stimulating stem cell differentiation to produce neural cells in the midbrain," said Andy Yang, first author on the study and a PhD student at the Donnelly Centre. "Moreover, cells activated via the FZD5 receptor closely resemble dopaminergic neurons of natural origin." Another promising finding of the study was that implanting the artificially-produced neurons in a rodent model with Parkinson's disease led to improvement of the rodent's locomotive impairment. "Our next step would be to continue using rodent or other suitable models to compare the outcomes of activating the FZD5 receptor and inhibiting GSK3," said Yang. "These experiments will confirm which method is more effective in improving symptoms of Parkinson's disease ahead of clinical trials." This research was supported by the University of Toronto Medicine by Design program, which receives funding from the Canada First Research Excellence Fund, and the Canadian Institutes of Health Research.

100 Deals associated with [11C]OCM-44

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Indication	Highest Phase	Country/Location	Organization	Date
Alzheimer Disease	Preclinical	United States	Pfizer Inc.	-
Alzheimer Disease	Preclinical	United States	Centre for Addiction & Mental Health	-
Alzheimer Disease	Preclinical	United States	Biogen, Inc.	-
Alzheimer Disease	Preclinical	United States	The University of Michigan-Dearborn	-

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