Last update 01 Nov 2024

CIT

Last update 01 Nov 2024

Basic Info

Synonyms

CIT, CITK, citron (rho-interacting, serine/threonine kinase 21)

+ [7]

Introduction

Plays a role in cytokinesis. Required for KIF14 localization to the central spindle and midbody. Putative RHO/RAC effector that binds to the GTP-bound forms of RHO and RAC1. It probably binds p21 with a tighter specificity in vivo. Displays serine/threonine protein kinase activity. Plays an important role in the regulation of cytokinesis and the development of the central nervous system. Phosphorylates MYL9/MLC2.

Drugs associated with CIT

C3TD879

Target

ACL x CIT

Mechanism

ACL inhibitors [+1]

Active Org.

Cleveland Clinic Lerner Research Institute [+1]

Originator Org.

Cleveland Clinic Lerner Research Institute

Active Indication

Neoplasms

Inactive Indication-

Drug Highest PhasePreclinical

First Approval Ctry. / Loc.-

First Approval Date20 Jan 1800

100 Clinical Results associated with CIT

100 Translational Medicine associated with CIT

0 Patents (Medical) associated with CIT

415

Literatures (Medical) associated with CIT

01 Jan 2025·Food Chemistry

Citral: A potent inhibitor of advanced glycation end products

Article

Author: Hu, Xiaosong ; Lin, Mengyi ; Zhu, Yuchen ; Hou, Kangdi ; Yang, Xin ; Wei, Siyu ; Chen, Fang ; Wei, Yumeng

Advanced glycation end products (AGEs), which are produced during food processing, pose health risks to humans. This study found that citral (Cit) effectively inhibited the formation of both fluorescent and non-fluorescent AGEs in the bovine serum albumin (BSA)-glucose (Glc) system. Cit achieved an average inhibition rate of over 80 % for fluorescent AGEs and reduced the levels of N-ε-carboxymethyllysine (CML) and N-ε-carboxyethyllysine (CEL) by up to 45.85 % and 59.32 %, respectively. The comprehensive characterizations and high-resolution mass spectrometry analysis demonstrated that the carbonyl group and CC group present on Cit could compete with Glc for the amino groups on BSA, thereby reducing the formation of AGEs. Additionally, the cytotoxicity assay demonstrated that the BSA-Cit adducts were non-toxic. This research indicated that Cit was a potent and safe inhibitor of AGEs.

01 Dec 2024·Bioresource Technology

Enhanced degradation of exogenetic citrinin by glycosyltransferases in the oleaginous yeast Saitozyma podzolica zwy-2-3

Article

Author: Xu, Hui ; Zeng, Jie ; Cao, Yi ; Yang, Qingzhuoma ; Qiao, Dairong ; Guo, Shengtao ; Ran, Yulu

The contamination by the toxin citrinin (CIT), produced by fungi, has been reported in agricultural foods and is known to be nephrotoxic to humans. In this study, we found that CIT could be effectively degraded by the oleaginous yeast Saitozyma podzolica zwy-2-3. Four genes encoding glycosyltransferases (GTs) in S. podzolica zwy-2-3 (SPGTs) were identified by evolutionary and structural analyses. The overexpression of SPGTs enhanced CIT degradation to 0.56 mg/L/h in S. podzolica zwy-2-3 by increasing ATP and glutathione (GSH) contents to oxidize CIT and scavenge reactive oxygen species (ROS). Besides, SPGTs promoted lipid synthesis by 9.3 % of S. podzolica zwy-2-3 under CIT stress. These results suggest that SPGTs in oleaginous yeast play a pivotal role in enhancing CIT degradation and lipid accumulation. These findings provide a valuable basis for the application of GTs in oleaginous yeast to alleviate CIT contamination in agricultural production, which may contribute to food safety.

01 Dec 2024·Gynecologic Oncology

Cold ischemia time and formalin fixation time in endometrial cancer: Should breast cancer guidelines for preanalytical variables be applied to hysterectomy specimens?

Article

Author: Kistenfeger, Quinn ; Haight, Paulina J. ; Leipold, Chelsea ; Lammers, Sydney ; Bixel, Kristin L. ; Bixel, Kristin L ; Suarez, Adrian A. ; Haight, Paulina J ; Tozbikian, Gary H. ; Esnakula, Ashwini ; Suarez, Adrian A ; Cosgrove, Casey ; Tozbikian, Gary H

OBJECTIVESThe American Society of Clinical Oncology (ASCO)/College of American Pathologists (CAP) recommend cold ischemia time (cIT) be <60 min, and formalin fixation time (FFT) 6-72 h, to optimize immunohistochemistry (IHC) based on breast cancer data. We assessed whether cIT and FFT impact IHC in endometrial cancer (EC), and determined which factors affect cIT and FFT.METHODSSurgical EC cases from 2019 to 2023 were reviewed. cIT was calculated by subtracting time of tissue devascularization intra-operatively from time the specimen was placed in formalin. Demographics, clinicopathologic and peri-operative factors, and IHC for estrogen receptor (ER), progesterone receptor (PR), human epidermal growth factor receptor 2 (HER2), and mismatch repair (MMR) proteins were compared between patients with cIT <60 min versus ≥60 min (prolonged), and compliant FFT (6-72 h) versus non-compliant FFT (<6 or > 72 h). Categorical variables were compared using χ² tests.RESULTS941 patients were included in the analysis. Median cIT was 33 min. Prolonged cIT occurred in 95 (10 %) cases. African American/Black race (p < 0.001), advanced stage (p < 0.001), mini-laparotomy (p < 0.001), performance of surgical procedures beyond standard EC staging (p < 0.001), longer surgical length (p < 0.001), and increased uterine weight (p < 0.001) were independently associated with prolonged cIT. There were no significant differences in ER, PR, HER2, or MMR protein expression based on cIT or FFT.CONCLUSIONProlonged cIT was not associated with differences in biomarker expression via IHC at time of surgical staging for EC. Despite variability in cIT, which is largely due to non-modifiable factors, tumor molecular features remain consistent and can reliably be utilized for prognostic and therapeutic decision-making.

News (Medical) associated with CIT

09 Mar 2023

·www.sciencedaily.com

New insights into cellular 'bridges' shed light on development, disease

Most cells in the bodies of living things duplicate their contents and physically separate into new cells through the process of cell division. But across many species, germ cells, those that become eggs or sperm, don't fully separate. They remain interconnected through small bridges called ring canals and cluster together. In a new study, researchers uncover how it is that germ cells in fruit flies form these ring canals, a finding that they say will provide new insights into a widely shared feature of development and into diseases in which cell division is disrupted. Most cells in the bodies of living things duplicate their contents and physically separate into new cells through the process of cell division. But across many species, germ cells, those that become eggs or sperm, don't fully separate. They remain interconnected through small bridges called ring canals and cluster together. In a new study, Yale researchers uncover for the first time how it is that germ cells in fruit flies form these ring canals, a finding that they say will provide new insights into a widely shared feature of development and into diseases in which cell division is disrupted. The findings were published March 9 in Developmental Cell. Scientists have observed ring canals in male and female germ cells across all types of species, from simpler organisms like sponges and fruit flies to more complex animals like mice and humans. And while their purpose is not fully understood, there is evidence that ring canals are important for cell development, the researchers say. "For example, in female fruit flies, ring canals are required to grow a functional oocyte, a developing egg cell," said Lynn Cooley, the C.N.H. Long Professor of Genetics at Yale School of Medicine and senior author of the new study. "If you block ring canals, female flies grow tiny, little eggs and can't reproduce." But how ring canals form has remained unclear. To better understand their formation, the researchers used a live imaging approach. They tagged several ring canal proteins in fruit flies with florescent molecules and, using a microscope, observed what those proteins did over time in the germ cells of both males and females. "When we did this, we saw the first signs of a structure we call the germline midbody," said Kari Price, a postdoctoral fellow in Cooley's lab and lead author of the study. The midbody is a structure that forms during cell division and one of its roles is to recruit the molecules needed to sever cells at the end of the process. In the study, the researchers found that an unusually large midbody formed in fruit fly germ cells, stuck around for about 20 to 30 minutes, and then, instead of initiating full separation, underwent dramatic remodeling from a sphere into a ring. These midbody rings then became stable ring canals that connected the sibling cells. The researchers also found this midbody-to-ring canal transition in fresh-water polyps and mice, suggesting it's a feature that has been preserved throughout evolution. "To see this solid, little object turn into a ring -- that had not been observed in intact living cells before. It was, to us, very striking; it was an 'a-ha moment,'" said Cooley. "And it would've been tough to discover this in anything other than fruit flies. This study is such a great example of how model systems like fruit flies are essential for understanding fundamental mechanisms of development." In addition to being an important step toward understanding the function and formation of ring canals, the researchers say, the new discovery may also yield insight into incomplete cell division that occurs in typical development across a variety of species and into diseases where incomplete cell division is implicated, such as colorectal cancer, Hodgkin's lymphoma, and some immunodeficiency syndromes. The findings may also help scientists understand the very beginnings of evolution. "There are very primitive creatures that, when they divide, make colonies that are attached with persistent cellular bridges, much like what we see with germ cells," said Cooley. "Maybe this way of keeping sibling cells connected in a colony or cluster is the beginning of how multicellular evolution occurred, and maybe germ cells are a reflection of that." Going forward, the researchers aim to identify the mechanisms that drive germ cells to remain connected. "In this current study we saw that blocking an enzyme called Citron kinase delayed or prevented the midbody-to-ring canal transition," said Price. "So we're looking at Citron kinase more deeply to see what exactly it's doing in these cells during division."

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