The team integrates experimental analyses of clinical and basic medicine and transgenic mice models. miR-29a acts a potent protective factor against excessive fibrosis in myofibroblasts of subacromial bursa tissue. Gain of miR-29a stabilizes tendon and synovial tissue homeostasis that alleviates tissue stiffness and maintains function.

Start Date01 Aug 2014

Sponsor / Collaborator

Chang Gung Memorial Hospital

100 Clinical Results associated with MicroRNA-29

100 Translational Medicine associated with MicroRNA-29

100 Patents (Medical) associated with MicroRNA-29

261

Literatures (Medical) associated with MicroRNA-29

01 Jun 2025·INTERNATIONAL IMMUNOPHARMACOLOGY

miR-29a nanoparticles improve chronic insomnia by regulating microglia activation and hippocampal neuronal cell pyroptosis through PER2/NF-κB axis

Article

Author: Hou, Dan ; Hu, Yujie ; Yang, Guoshuai ; Li, Hongxin

OBJECTIVE:

Chronic insomnia can easily lead to clinical distress or cause mental, social, physical, educational, occupational, or other functional impairments. Considering the role of circadian rhythm in insomnia, we focused on exploring the action of miR-29a in regulating the PER2 gene in improving chronic insomnia.

METHODS:

LPS induces the expression of miRNAs targeting PER2 in HMC3 and PRM cells, which was verified by RT-qPCR. Poly-lactic-co-glycolic acid (PLGA) nanoparticles (NP) were used to encapsulate short hairpin (sh)-miR-29a to construct sh-miR-29a-NP. Morris water environment method was employed to establish a sleep deprivation rat model to investigate the therapeutic effects of sh-miR-29a-NP. Cell viability and levels of cell polarization factors were evaluated using CCK8 and ELISA, respectively. The Morris water maze test was applied to assess the learning and memory capabilities of the rats. Immunohistochemistry, immunofluorescence, and western blot were applied to test the expression of glial cell polarization, neuronal cell activation, apoptosis, and Period2 (PER2) /nuclear factor kappa B (NF-κB) axis proteins.

RESULTS:

miR-29a was significantly upregulated in LPS-induced HMC3 and PRM cells, with the most significantly altered miRNAs/PER2 interaction. In LPS-induced HMC3 and PRM cells, sh-miR-29a promoted the PER2 and CD206 expressions, and inhibited the expression of ionized calcium-binding adaptor molecule 1 (IBA-1), NF-κB, and CD86, while this effect was blocked by small interfering-PER2. Further in vivo experiments confirmed that PER2 and CD206 expression was reduced, while NF-κB, CD86, and IBA-1 expression were up-regulated in the hippocampal tissue of CSD rats. However, this effect was reversed by treatment with sh-miR-29a-NP. Treatment with sh-miR-29a-NP in CSD rats shortened the escape latency and increased the number of crossings over the original platform, while inhibited the expression of NLR Family Pyrin Domain Containing 3, caspase-1, Gasdermin D (GSDMD), and TUNEL signal in the hippocampal tissue.

CONCLUSION:

The regulation of PER2/NF-κB pathway by sh-miR-29a-NP promoted M2 polarization of microglial cells and inhibited neuronal cell pyroptosis, thereby improving cognitive dysfunction in chronic insomnia.

01 Jan 2025·BIOCHIMICA ET BIOPHYSICA ACTA-MOLECULAR BASIS OF DISEASE

MicroRNAs and human viral diseases: A focus on the role of microRNA-29

Review

Author: Taghavi, Seyed Pouya ; Hashemian, Seyed Mohammad Reza ; Kermanshahi, Atefeh Zamani ; Baghi, Hossein Bannazadeh ; Lotfalizadeh, Mohammad Hassan ; Ravaei, Fatemeh ; Bayat, Mobina ; Kobravi, Sepehr ; Kesheh, Mina Mobini ; Mirzaei, Hamed ; Heydari, Azhdar ; Memar, Mohammad Yousef ; Nahand, Javid Sadri ; Zarepour, Fatemeh

The viral replication can impress through cellular miRNAs. Indeed, either the antiviral responses or the viral infection changes through cellular miRNAs resulting in affecting many regulatory signaling pathways. One of the microRNA families that is effective in human cancers, diseases, and viral infections is the miR-29 family. Members of miR-29 family are effective in different viral infections as their roles have appeared in regulation of immunity pathways either in innate immunity including interferon and inflammatory pathways or in adaptive immunity including activation of T-cells and antibodies production. Although miR-29a affects viral replication by suppressing antiviral responses, it can inhibit the expression of viral mRNAs via binding to their 3'UTR. In the present work, we discuss the evidence related to miR-29a and viral infection through host immunity regulation. We also review roles of other miR-29 family members by focusing on their role as biomarkers for diagnosing and targets for viral diseases management.

01 Jan 2025·JOURNAL OF MOLECULAR GRAPHICS & MODELLING

How a mixture of microRNA-29a (miR-29a) and microRNA-144 (miR-144) cancer biomarkers interacts with a graphene quantum dot

Article

Author: Awang, Tadsanee ; Traiphothon, Darunee ; Kuntip, Nattapon ; Japrung, Deanpen ; Pongprayoon, Prapasiri

MicroRNAs (miRNAs) which are small non-coding RNAs have been reported to be potential cancer biomarker. However, it is difficult to extract such short RNA from a sample matrix. New effective strategies are required. Recently, graphene quantum dots (GQDs) have been used to detect nucleotides in many biosensor platforms, but their applications for miRNA extraction remain limited. GQD was reported to be able to collect short miRNA, but its performance to collect miRNAs with different structure remains unknown. Thus, in this work, the capability of GQD to interact with two different miRNAs is investigated. A mixture of hairpin-like miR-29a and circular miR-144 molecules are used as a representative of two miRNA morphologies. Two systems (a miRNA mixture, comprising 4 of miR-29a and 4 of miR-144, with (miR_GQD) and without GQD (miR)) were studied in comparison. MiRNAs in a mixture (miR) can aggregate, but no permanent miRNA assembly is captured. In contrast, the presence of GQD can rapidly and spontaneously activate the permanent miRNA/GQD clustering. This finding highlights the ability of GQD to be a miRNA collector. Interestingly, all GQD-bound miRNAs do not unfold. This allows the easy accessibility for probes. Also, nano-sized GQD seems to prefer hairpin miR-29a. The free 5' terminus of miR-29a acts as the sticky end to adhere on GQD. This work highlights the importance of RNA secondary structure on GQD/miRNA aggregation capability. An insight obtained here will be useful for further design of miRNA isolation strategies.

News (Medical) associated with MicroRNA-29

01 Feb 2024

·www.sciencedaily.com

Small RNAs take on the big task of helping skin wounds heal better and faster with minimal scarring

New findings report that a class of small RNAs (microRNAs), microRNA-29, can restore normal skin structure rather than producing a wound closure by a connective tissue (scar). Any improvement of normal skin repair would benefit many patients affected by large-area or deep wounds prone to dysfunctional scarring. New findings in The American Journal of Pathology, published by Elsevier, report that a class of small RNAs (microRNAs), microRNA-29, can restore normal skin structure rather than producing a wound closure by a connective tissue (scar). Any improvement of normal skin repair would benefit many patients affected by large-area or deep wounds prone to dysfunctional scarring. Because the burden of non-healing wounds is so significant, it is sometimes called a "silent pandemic." Worldwide, costs associated with wound care are expected to reach US$15 to 22 billion per year by 2024, exceeding the cost of managing obesity-related health problems in some parts of the world. Lead investigator Svitlana Kurinna, PhD, Division of Cell Matrix Biology and Regenerative Medicine, FBMH, University of Manchester, explained, "We had data showing that microRNAs can regulate skin growth. microRNAs do not code for proteins, so it wasn't clear exactly how such small molecules can make changes to the skin. We therefore studied underlying mechanisms that could be targeted to improve cutaneous wound healing." The molecular events during early wound healing stages of inflammation and tissue formation have been well described using single cell sequencing and proteomic approaches. microRNAs are important factors in healing and may regulate functions in skin repair; however, the mechanisms underlying tissue remodeling are unclear. Scientists studying wound healing in microRNA-29 gene knockout transgenic mice suggest that the release of microRNA-29 targets promotes wound healing by regulating skin regeneration by binding long RNAs coding for structural protein laminin C2 (LAMC2) of the skin. This restores the normal skin structure rather than creating a connective tissue scar. In the current study, researchers noted that wild type wounded mice healed quite well, but the skin of transgenic mice devoid of microRNA-29 regenerated even better. To understand the reasons, they conducted in-depth microscopic analysis of the transgenic wounds. They observed deposition of LAMC2 -- usually found in one of the skin layers in wild mice -- around blood vessels inside the wounds of microRNA-29-deficient transgenic mice. This observation indicates that microRNA-29 may be inhibiting the expression of LAMC2, and deletion in the transgenic mice relieved the inhibition, which resulted in faster wound healing. Dr. Kurinna noted, "These processes are likely mediated by microRNA-29 target microRNAs released upon removal of microRNA-29 to improve cell matrix adhesion. These results further suggest a link between LAMC2, improved angiogenesis, and re-epithelialization. We had expected a different change in skin regeneration; we thought the removal of microRNA-29 would help outer layers of the skin to grow faster, but it was the deep matrix of the wound that showed an improvement. These findings in both mice and humans demonstrate the role of microRNA-29 in epidermal repair and suggest that the release of microRNA-29 targets, particularly LAMC2, promotes wound healing. The inhibition of microRNA-29 and/or overexpression of LAMC2 may be a new and effective strategy for improving wound healing. Dr Kurinna concluded, "Our findings are of particular interest because they show the mechanism to restore normal skin structure rather than a wound closure by a connective tissue (scar). Any improvement of normal skin repair would therefore help many patients affected by large-area or deep wounds prone to dysfunctional scarring."

14 Sep 2021

·www.biospace.com

Pancreatic Cancer Research Ramps Up as Roche and NovoCure Announce Partnership

Pancreatic cancer has the lowest survival rate of the most common cancers, less than 10% of patients survive longer than five years, largely due to most cases being diagnosed at a late stage. A collaboration between NovoCure and Roche hopes to improve those odds. This morning, NovoCure and Swiss pharma giant Roche announced a collaboration to develop Tumor Treating Fields (TTFields) in combination with Roche’s anti-PD-L1 therapy, atezolizumab, for patients diagnosed with metastatic pancreatic ductal adenocarcinoma (mPDAC). This is the most common form of pancreatic cancer, accounting for 85%–95% of all solid pancreatic tumors. NovoCure and Roche aim to explore the combined efficacy of TTFields with atezolizumab as a potential treatment for pancreatic cancer. TTFields, are electric fields that disrupt cancer cell division. William Dole, executive chairman of NovoCure, said the immune-shielded environment of the pancreas has been challenging for immunotherapeutics as a monotherapy treatment. Dole said the Phase II pilot study will assess the ability of TTFields combined with atezolizumab to improve clinical outcomes for patients with this disease. NovoCure said TTFields are primarily intended for use combined with other standard-of-care cancer treatments. The Phase II study will assess the combination of TTFields together with atezolizumab, gemcitabine and nab-paclitaxel as a first-line treatment for mPDAC. The primary endpoint of the study is disease control rate. Secondary endpoints will include overall survival, progression free survival, one year survival, objective response rate, PFS at six months, duration of response, and toxicity profile. While Roche and NovoCure work on their potential therapeutic, researchers at Indiana University’s Melvin and Bren Simon Comprehensive Cancer Center are taking a different approach. Scientists have noted the restoration of a missing molecule in pancreatic fibrosis could improve the delivery of other treatments aimed at the deadly disease. Fibrosis in the pancreas often results from damage caused by pancreatic cancer and chronic pancreatitis. Janaiah Kota, an assistant professor of medical and molecular genetics at the university’s medical school and a researcher at the cancer center, said the cancer cells develop a fibrotic tissue around the cells, which is a major barrier for drug delivery. Kota and colleagues discovered that a molecule known as microRNA-29a (miR-29a) “functions as an anti-fibrosis and anti-inflammatory in the pancreas.” Including this molecule in drug therapy overcome the fibrotic barrier for treatment, they said. There are no FDA-approved therapies to reduce fibrosis in pancreatic cancer. The research team established the role of miR-29a as a therapeutic agent in mouse models. Findings of the discovery were posted in JCI Insights. Moving forward, Kota and the IU research team are assessing the use of adeno-associated virus gene therapy technology to restore the missing molecule in the pancreas. “This tiny molecule is missing in the pancreas and, more broadly, the fibrotic tissue. When we put this molecule back in cells, it significantly reduces the potential for cancer cells to develop fibrotic tissue around the tumors,” Kota said in a statement.

CollaborateSmall molecular drugGene Therapy

14 Sep 2021

·www.biospace.com

Pancreatic Cancer Research Ramps Up as Roche and NovoCure Announce Partnership

NovoCure and Roche aim to explore the combined efficacy of TTFields with atezolizumab as a potential treatment for pancreatic cancer. Pancreatic cancer has the lowest survival rate of the most common cancers, less than 10% of patients survive longer than five years, largely due to most cases being diagnosed at a late stage. A collaboration between NovoCure and Roche hopes to improve those odds. This morning, NovoCure and Swiss pharma giant Roche announced a collaboration to develop Tumor Treating Fields (TTFields) in combination with Roche’s anti-PD-L1 therapy, atezolizumab, for patients diagnosed with metastatic pancreatic ductal adenocarcinoma (mPDAC). This is the most common form of pancreatic cancer, accounting for 85%–95% of all solid pancreatic tumors. NovoCure and Roche aim to explore the combined efficacy of TTFields with atezolizumab as a potential treatment for pancreatic cancer. TTFields, are electric fields that disrupt cancer cell division. William Dole, executive chairman of NovoCure, said the immune-shielded environment of the pancreas has been challenging for immunotherapeutics as a monotherapy treatment. Dole said the Phase II pilot study will assess the ability of TTFields combined with atezolizumab to improve clinical outcomes for patients with this disease. NovoCure said TTFields are primarily intended for use combined with other standard-of-care cancer treatments. The Phase II study will assess the combination of TTFields together with atezolizumab, gemcitabine and nab-paclitaxel as a first-line treatment for mPDAC. The primary endpoint of the study is disease control rate. Secondary endpoints will include overall survival, progression free survival, one year survival, objective response rate, PFS at six months, duration of response, and toxicity profile. While Roche and NovoCure work on their potential therapeutic, researchers at Indiana University ’s Melvin and Bren Simon Comprehensive Cancer Center are taking a different approach. Scientists have noted the restoration of a missing molecule in pancreatic fibrosis could improve the delivery of other treatments aimed at the deadly disease. Fibrosis in the pancreas often results from damage caused by pancreatic cancer and chronic pancreatitis. Janaiah Kota, an assistant professor of medical and molecular genetics at the university’s medical school and a researcher at the cancer center, said the cancer cells develop a fibrotic tissue around the cells, which is a major barrier for drug delivery. Kota and colleagues discovered that a molecule known as microRNA-29a (miR-29a) “functions as an anti-fibrosis and anti-inflammatory in the pancreas.” Including this molecule in drug therapy overcome the fibrotic barrier for treatment, they said. There are no FDA-approved therapies to reduce fibrosis in pancreatic cancer. The research team established the role of miR-29a as a therapeutic agent in mouse models. Findings of the discovery were posted in JCI Insights . Moving forward, Kota and the IU research team are assessing the use of adeno-associated virus gene therapy technology to restore the missing molecule in the pancreas. “This tiny molecule is missing in the pancreas and, more broadly, the fibrotic tissue. When we put this molecule back in cells, it significantly reduces the potential for cancer cells to develop fibrotic tissue around the tumors,” Kota said in a statement.

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100 Deals associated with MicroRNA-29

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Indication	Highest Phase	Country/Location	Organization	Date
Glaucoma	Preclinical	Taiwan Province	Wenzhou Medical College	08 Nov 2022

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