Keyword search (4,163 papers available)

"Piekny A" Authored Publications:

Title Authors PubMed ID
1 Open-space microfluidics as a tool to study signaling dynamics Proulx M; Clapperton-Richard P; Potvin-Trottier L; Piekny A; Gervais T; 40995884
BIOLOGY
2 Surface charge dictates the mechanism of cellular uptake of fluorescent amine passivated carbon dots Clermont-Paquette A; Fuoco G; Brancheriau CR; Piekny A; Naccache R; 40861971
CHEMBIOCHEM
3 Development of dual acid-visible light-degradable core-crosslinked nanogels with extended conjugate aromatic imines for enhanced drug delivery Bairagi K; Shamekhi M; Tountas I; Letourneau N; Peslherbe GH; Piekny A; Oh JK; 40637173
BIOLOGY
4 Endogenous tagging using split mNeonGreen in human iPSCs for live imaging studies Husser MC; Pham NP; Law C; Araujo FRB; Martin VJJ; Piekny A; 38652106
BIOLOGY
5 Advances in the design and use of carbon dots for analytical and biomedical applications Adeola AO; Clermont-Paquette A; Piekny A; Naccache R; 37757783
CHEMBIOCHEM
6 Ratiometric Sensing of Glyphosate in Water Using Dual Fluorescent Carbon Dots Clermont-Paquette A; Mendoza DA; Sadeghi A; Piekny A; Naccache R; 37299928
BIOLOGY
7 Diversity is the spice of life: An overview of how cytokinesis regulation varies with cell type Ozugergin I; Piekny A; 36420142
BIOLOGY
8 Gold Nano-Bio-Interaction to Modulate Mechanobiological Responses for Cancer Therapy Applications Sohrabi Kashani A; Larocque K; Piekny A; Packirisamy M; 35839330
BIOLOGY
9 Diverse mechanisms regulate contractile ring assembly for cytokinesis in the two-cell C. elegans embryo Ozugergin I; Mastronardi K; Law C; Piekny A; 35022791
BIOLOGY
10 Characterization of a recently synthesized microtubule-targeting compound that disrupts mitotic spindle poles in human cells Jaunky DB; Larocque K; Husser MC; Liu JT; Forgione P; Piekny A; 34880347
BIOLOGY
11 Design, structure-activity relationship study and biological evaluation of the thieno[3,2-c]isoquinoline scaffold as a potential anti-cancer agent Liu JT; Jaunky DB; Larocque K; Chen F; Mckibbon K; Sirouspour M; Taylor S; Shafeii A; Campbell D; Braga H; Piekny A; Forgione P; 34416378
BIOLOGY
12 Seeing is believing: tools to study the role of Rho GTPases during cytokinesis Koh SP; Pham NP; Piekny A; 34405757
BIOLOGY
13 Using intracellular plasmonics to characterize nanomorphology in human cells. Sohrabi Kashani A, Piekny A, Packirisamy M 33365137
BIOLOGY
14 Multi-tissue patterning drives anterior morphogenesis of the C. elegans embryo. Grimbert S, Mastronardi K, Richard V, Christensen R, Law C, Zardoui K, Fay D, Piekny A 33309948
BIOLOGY
15 Anillin Controls the Rho Zone. Piekny A 32893380
BIOLOGY
16 Importin-binding mediates the intramolecular regulation of anillin during cytokinesis. Beaudet D, Pham N, Skaik N, Piekny A 32238082
BIOLOGY
17 Complementary functions for the Ran gradient during division. Ozugergin I, Piekny A 32013678
BIOLOGY
18 Active Ran regulates anillin function during cytokinesis. Beaudet D, Akhshi T, Phillipp J, Law C, Piekny A 28931593
BIOLOGY
19 Dual disassembly and biological evaluation of enzyme/oxidation-responsive polyester-based nanoparticulates for tumor-targeting delivery. Hong SH, Larocque K, Jaunky DB, Piekny A, Oh JK 30223243
CHEMBIOCHEM

 

Title:Characterization of a recently synthesized microtubule-targeting compound that disrupts mitotic spindle poles in human cells
Authors:Jaunky DBLarocque KHusser MCLiu JTForgione PPiekny A
Link:https://pubmed.ncbi.nlm.nih.gov/34880347/
DOI:10.1038/s41598-021-03076-3
Publication:Scientific reports
Keywords:
PMID:34880347 Category: Date Added:2021-12-09
Dept Affiliation: BIOLOGY
1 Department of Biology, Concordia University, Montreal, QC, Canada.
2 Department of Chemistry and Biochemistry, Concordia University, Montreal, QC, Canada.
3 Department of Biology, Concordia University, Montreal, QC, Canada. alisa.piekny@concordia.ca.

Description:

We reveal the effects of a new microtubule-destabilizing compound in human cells. C75 has a core thienoisoquinoline scaffold with several functional groups amenable to modification. Previously we found that sub micromolar concentrations of C75 caused cytotoxicity. We also found that C75 inhibited microtubule polymerization and competed with colchicine for tubulin-binding in vitro. However, here we found that the two compounds synergized suggesting differences in their mechanism of action. Indeed, live imaging revealed that C75 causes different spindle phenotypes compared to colchicine. Spindles remained bipolar and collapsed after colchicine treatment, while C75 caused bipolar spindles to become multipolar. Importantly, microtubules rapidly disappeared after C75-treatment, but then grew back unevenly and from multiple poles. The C75 spindle phenotype is reminiscent of phenotypes caused by depletion of ch-TOG, a microtubule polymerase, suggesting that C75 blocks microtubule polymerization in metaphase cells. C75 also caused an increase in the number of spindle poles in paclitaxel-treated cells, and combining low amounts of C75 and paclitaxel caused greater regression of multicellular tumour spheroids compared to each compound on their own. These findings warrant further exploration of C75's anti-cancer potential.





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