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Last update 08 May 2025

PDE6D

Last update 08 May 2025

Basic Info

Synonyms

GMP-PDE delta, JBTS22, PDE6D

+ [5]

Introduction

Promotes the release of prenylated target proteins from cellular membranes (PubMed:9712853). Modulates the activity of prenylated or palmitoylated Ras family members by regulating their subcellular location (PubMed:22002721, PubMed:23698361). Required for normal ciliary targeting of farnesylated target proteins, such as INPP5E (PubMed:24166846). Modulates the subcellular location of target proteins by acting as a GTP specific dissociation inhibitor (GDI) (By similarity). Increases the affinity of ARL3 for GTP by several orders of magnitude. Stabilizes ARL3-GTP by decreasing the nucleotide dissociation rate (By similarity).

Drugs associated with PDE6D

FPFT-2216

Target

CK1α x IKZF1 x IKZF3 x PDE6D

Mechanism

CK1α inhibitors [+3]

Active Org.

Osaka University Immunology Frontier Research Center (IFREC)

Originator Org.

Osaka University Immunology Frontier Research Center (IFREC)

Active Indication

Myelodysplastic Syndromes

Inactive Indication-

Drug Highest PhasePreclinical

First Approval Ctry. / Loc.-

First Approval Date20 Jan 1800

Deltaflexin-3

Target

PDE6D

Mechanism

PDE6D inhibitors

Active Org.

University of Luxembourg

Originator Org.

University of Luxembourg

Active Indication

Neoplasms

Inactive Indication-

Drug Highest PhasePreclinical

First Approval Ctry. / Loc.-

First Approval Date20 Jan 1800

C14(Instituto Politecnico Nacional)

Target

KRAS G13D x PDE6D

Mechanism

KRAS G13D modulators [+1]

Active Org.

Instituto Politecnico Nacional

Originator Org.

Instituto Politecnico Nacional

Active Indication

Triple Negative Breast Cancer

Inactive Indication-

Drug Highest PhasePreclinical

First Approval Ctry. / Loc.-

First Approval Date20 Jan 1800

100 Clinical Results associated with PDE6D

100 Translational Medicine associated with PDE6D

0 Patents (Medical) associated with PDE6D

150

Literatures (Medical) associated with PDE6D

01 Apr 2025·Cancer Letters

Metformin inhibits the progression of castration resistant prostate cancer by regulating PDE6D induced purine metabolic alternation and cGMP / PKG pathway activation

Article

Author: Tan, Zeheng ; Tang, Zhenfeng ; Deng, Yulin ; Tian, Weicheng ; Feng, Yuanfa ; Zou, Zhihao ; Wen, Biyan ; Zhong, Weide ; Ye, Jianheng ; Wu, Yongding ; Zhu, Xuejin ; Wu, Zhenjie ; Cai, Shanghua ; Han, Zhaodong ; Xiao, Haiyin ; Liu, Ren ; He, Huichan ; Li, Jinchuang

The castration-resistant prostate cancer (CRPC) remains an incurable disease. Metformin has demonstrated a potential therapeutic effect on CRPC. However, the poor clinical performance of metformin against cancer may be due to its clinical dose being much lower than the anticancer concentration used in pre-clinical experiments. The challenge is to determine a way to enhance sensitivity to metformin at an appropriate concentration on CRPC. In this study, a mouse model of low-dose metformin treatment for CRPC cells were established. Metabolomic-seq and transcriptomic-seq was used to investigate changes in CRPC xenografts. We discovered that low-dose metformin inhibits the progression of CRPC by regulating PDE6D, which induces alterations in purine metabolism and activates the cGMP/PKG pathway. Furthermore, we found that cells with high expression of PDE6D were more resistant to metformin. When combined with the PDE6D inhibitor TMX-4100, the inhibitory effect on tumors was enhanced, and TMX-4100 demonstrated favorable biosafety in animal models. In conclusion, we found that low-dose metformin inhibits the progression of CRPC by regulating PDE6D-induced alterations in purine metabolism and activating the cGMP/PKG pathway. Moreover, patients with high PDE6D expression may exhibit greater resistance to metformin. Combining metformin with TMX-4100 could further improve the inhibitory effects on tumors.

01 Mar 2025·Animal Bioscience

Genome-wide copy number variation regions in indigenous (Bos indicus) cattle breeds of Tamil Nadu, India

Article

Author: Vani, S ; S, Vani ; Gopinathan, A ; Balasubramanyam, D ; Karthickeyan, S M K ; D, Balasubramanyam ; A, Gopinathan ; SMK, Karthickeyan ; Tirumurugaan, K G ; KG, Tirumurugaan

Objective: Identification of large scale structural polymorphisms (copy number variations [CNVs]) of more than 50 bp between the individuals of a species would help in knowing genetic diversity, phenotypic variability, adaptability to tropical environment and disease resistance.Methods: Read depth-based method implemented in CNVnator was used for calling copy number variant regions on sequenced data obtained from whole-genome sequencing from 15 pooled samples belonging to five draught cattle breeds of Tamil Nadu.Results: A total of 11,605 CNV regions (CNVRs) were observed covering a genome size of 18.63 percent. Among these, 11,459 were restricted to autosomes, consisting of 11,013 deletions, 353 duplications and 93 complex events. These CNVRs were annotated to 4,989 candidate genes. A total of 8,291 numbers of CNVRs were shared among the five cattle breeds as also supported by principal component analysis and STRUCTURE analyses and 1,172 CNVRs were breed-specific. Four out of five selected breed-specific CNVRs were validated using real-time polymerase chain reaction. Genes with CNVRs are related to milk production (BTN1A1, ABCA1, and LAP3), disease resistance (TLR4 and DNAH8), adaptability (SOD1, CAST, and SMARCAL1), growth (EGFR, NKAIN3), reproduction (BRWD1 and PDE6D), meat and carcass traits (MAP3K5 and NCAM1) and exterior (ATRN and MITF) traits. Gene enrichment analysis based on the gene list retrieved from the CNVRs disclosed over-represented terms (p<0.01) associated with milk fat production. NETWORK analysis had identified 13 putative candidate genes involved in milk fat percentage, milk fat yield, lactation persistency, milk yield, heat tolerance, calving ease, growth and conformation traits.Conclusion: The genome-wide CNVRs identified in the present study produced genomewide partial CNV map in indigenous cattle breeds of Tamil Nadu.

01 Mar 2025·Biochemistry and Biophysics Reports

Single-cell RNAseq reveals adverse metabolic transcriptional program in intrahepatic cholangiocarcinoma malignant cells

Article

Author: Pineau, Pascal ; Desterke, Christophe ; Marchio, Agnès ; Mata-Garrido, Jorge ; Monge, Claudia ; Fu, Yuanji ; Francés, Raquel

Intrahepatic cholangiocarcinoma (ICA) is a highly aggressive primary liver cancer, which originates from the epithelial cells of the bile ducts. The transcriptional profile of metabolic enzymes was investigated at both bulk and single-cell levels in tumor samples from distinct ICA cohorts. In a training cohort (TCGA consortium), 16 genes encoding for metabolic enzymes were found overexpressed in cases with poor survival. A computed metabolic gene expression score was significantly associated with worse ICA prognosis at the univariate level (overall survival [OS] log-rank p = 8.2e-4). After adjusting for Ishak fibrosis score and tumor staging, the metabolic expression remained an independent predictor of poor prognosis (multivariate OS log-rank p = 0.01). Seven genes encoding key enzymes (FH, MAT2B, PLOD2, PLOD1, PDE6D, ALDOC, and NT5DC3) were validated as markers of the proliferative subclass of ICA in the GSE32225 dataset, related to poor prognosis. The metabolic score was significantly different between the inflammatory and proliferative subclasses in the validation cohort (p < 2.2e-16). At the single-cell level, in the tumor microenvironment of 10 ICA patients, these seven enzymes were predominantly expressed by malignant cells. The single-cell metabolic score was thus higher in malignant cells. This study identifies a metabolic transcriptional program linked to poor prognosis in ICA, independent of fibrosis and tumor staging.

News (Medical) associated with PDE6D

11 Dec 2023

·www.sciencedaily.com

New way to force pathogenic proteins into degradation

A number of diseases are caused by proteins that have spun out of control. Unfortunately, so far, conventional drugs have been able to stop only a fraction of these troublemakers. A new class of drugs known as PROTACs holds great promise in pharmaceutical research. They mark proteins for targeted degradation by the cell's own protein disposal system. Many diseases are caused by proteins that have spun out of control. Unfortunately, so far, conventional drugs have been able to stop only a fraction of these troublemakers. A new class of drugs known as PROTACs holds great promise in pharmaceutical research. They mark proteins for targeted degradation by the cell's own protein disposal system. Many of today's drugs are small, simple molecules. They usually work by regulating the activity of proteins involved in pathologically derailed processes—which is precisely what makes their development extremely complicated. Consequently, a highly adapted molecule has to be developed for each protein, to fit into the corresponding lock—the active center of the protein—like a high-security key. However, proteins actively involved in pathologically derailed processes make up only a fraction of the disease-related proteins. As a result, many proteins are still considered therapeutically “undruggable.” Cancer protein Ras—not undruggable after all? A majority of the undruggable proteins are compelling targets in cancer research. Perhaps the most prominent among them is the small Ras protein. A single small change in Ras is enough to irreversibly flip the switch for cell growth to “on”—with serious consequences: The cells proliferate rapidly and uncontrollably. Ras mutations occur in nearly a quarter of all tumors. In a groundbreaking study in 2013, a team of researchers led by Herbert Waldmann at MPI in Dortmund developed a new strategy to make Ras, which was previously considered undruggable, druggable: Instead of targeting Ras directly, the researchers used a specially developed molecule to thwart the auxiliary protein PDEd, manipulating the transport and thus the activity of Ras in the cell. However, the researchers did not manage to completely stop the cancer-driving activity of Ras. Two-armed molecule marks cancer protein for degradation Only two years after Waldmann's work, American researchers developed a promising new class of drugs to eliminate pathological proteins: they are known as PROTACs (proteolysis-targeting chimeras). These compounds effectively hijack the body's own protein waste removal system. The large molecule composed of two arms grabs the target protein on one side and the E3 ligase of the protein waste system on the other, which prompts the waste system to dispose of the pathological protein. “That’s an ingenious, truly outstanding scientific achievement,” says Waldmann. “Instead of inhibiting the target protein’s enzymatic activity in a complex process, PROTACs only need to bind to their target with high selectivity. Theoretically speaking, this principle is universally applicable to all proteins, including our Ras transporter PDEd, as we have successfully demonstrated in our current work,” he concludes. Serendipitous discovery opens up new possibilities The chemists Waldmann and Winter, along with their teams, created a new PROTAC consisting of the PDEd inhibitor they had developed. They linked the inhibitor to a well-studied molecule that is known to alert another degradation system which can also process larger cell components. “However, our screens have revealed that instead of activating what we call macroautophagy, our PROTAC activates the protein degradation system,” says Georg Winter. He goes on to explain: “What is particularly interesting is that our PROTAC binds a new ligase that was not accessible to the PROTAC strategy so far.” Currently, there are practically only two E3 ligases that can be used as binding sites for PROTACs. However, there are more than 600 E3 ligases in our bodies. And some of them are only present in very specific tissues. “Tissue-specific ligases could be used to specifically control the site of drug activity,” says Waldmann, looking to the future. “Our rather fortuitous discovery allows for further biological and medicinal-chemical investigation into the ligases we have found. This could help expand the range of pharmaceutically usable PROTACs and, one day, enable the targeted degradation of proteins in specific tissues,” he concludes.

PROTACs

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PDE6D

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