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Wikipedia

Pyr1

January 01, 1970

Pyr1 (LIMINIB) is an organic compound composed of carbon, hydrogen, oxygen and nitrogen that inhibits the enzyme LIM kinase.

Pyr1
Names
Preferred IUPAC name
5,11-Dimethyl-1-oxo-2,6-dihydro-1H-pyrido[4,3-b]carbazol-9-yl benzoate
Other names
LIMINIB
Identifiers
  • 83947-94-8 Y
3D model (JSmol)
  • Interactive image
ChemSpider
  • 61709937
  • 13074411
UNII
  • YL48YW74QQ Y
  • InChI=1S/C24H18N2O3/c1-13-17-10-11-25-23(27)21(17)14(2)20-18-12-16(8-9-19(18)26-22(13)20)29-24(28)15-6-4-3-5-7-15/h3-12,26H,1-2H3,(H,25,27)
    Key: BPGBAEXPBQHBSV-UHFFFAOYSA-N
  • O=C(C1=CC=CC=C1)OC(C=C2)=CC3=C2NC4=C3C(C)=C5C(C=CNC5=O)=C4C
Properties
C24H18N2O3
Molar mass 382.419 g·mol−1
Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa).

It was discovered by the Cure and Inserm Institute, CNRS and CEA in the 2010s. The studies in vitro and with animals,[1] prove that this molecule has a completely new mechanism of action that could be used against chemotherapy resistant cells.

Pyr1 reversibly stabilizes microtubules, blocks actin microfilament dynamics and inhibits cell motility in vitro. These characteristics confer not only anticancer properties but also the capacity to prevent metastasis to the molecule.

Description and properties edit

Pyr1 is classified as a small molecule that belongs to the group of pyridocarbazoles.[2] Its small size gives it special properties: as a light molecule it is a valuable tool for studying dynamic biological processes. Therefore, it is a key discovery in medical and biological investigation. It is a high degree protein temporal controller, as it is able to interact in a few minutes or even seconds with molecules such as LIMK1. Its reversibility enables it to quickly activate and inhibit itself, making the molecule a specific inhibitor both in vitro and in cellulo.

Pyr1 can be described as a tetracyclic molecule with a simple structure. Its few radicals are widely expanded along the benzene rings, distinguishing a benzoyloxy group in the ninth carbon and two methyl radicals in carbon five and eleven. There is also a ketone group in carbon one and two hydrogen radicals in carbons two and six.

Mechanism of action edit

Pyr 1 is a cell permeable competitive inhibitor of Lim Kinase (especially LIMK1). The latter is the enzyme that uses ATP to phosphorylate and inactivate the actin-depolymerizing factor cofilin. When cofilin is phosphorylated, it regulates actin dynamics. LIMK1 also depolymerizes microtubules.

 
Mechanism of action of LIMK1

In the presence of Pyr1, LIMK1 is inhibited, which means that the phosphorylation of cofilin decreases, which results in the blockage of the regulation of actin microfilaments dynamics and, therefore, the disorganization of microfilaments. It also causes the stabilization of microtubules. This inhibition is reversible.

In conclusion, Pyr1 inhibits cell motility and controls actin dynamics and stabilizes microtubules. These properties can be used in anticancer treatment.

 
Mechanism of action of Pyr1

Medical applications edit

Cancer metastasis consists in the fast and uncontrolled division of abnormal cells. Microtubules have a key role in mitosis: they generate the mitotic spindle assembly, which allows chromosome segregation and the cell division. Their stabilization leads to the inability of cells to reproduce or to their apoptosis. That is why microtubule targeting agents are, nowadays, powerful anticancer drugs. It also explains why tubulin is now considered as one of the most highly validated cancer targets.

These anticancer drugs have, however, some limitations due to side effects, principally myelosuppression and neurotoxicity. But the main inconvenience is that many cancers are, or become, resistant to these drugs. Several strategies have been proposed for the development of more effective and less toxic anticancer drugs. One of them is to use molecules that can induce the stabilization of microtubules, and Pyr1 is one of them.

Pyr1 may be used in cancer treatment, because its main target enzyme (LIM kinase) is a regulator of microtubule and actin dynamics. Moreover, it has been shown that Pyr1 is toxic for cancerous cell lines, even the ones that are resistant to conventional microtubule targeting agents.

Furthermore, the toxicity of Pyr1 has been studied in mice, to evaluate whether it could really work as a chemotherapeutic agent. The results show a complete survival of mice against xenografted tumors with no apparent toxicity, as there was no loss of weight observed. Therefore, it has been concluded that Pyr1 has a good therapeutic efficacy preventing tumor growth at doses that are well tolerated by animals.

Bearing the previous points in mind, Pyr1 may be used in addition or as an alternative to standard chemotherapy in drug resistant tumors.

References edit

  1. ^ Prudent, R.; Vassal-Stermann, E.; Nguyen, C.-H.; Pillet, C.; Martinez, A.; Prunier, C.; Barette, C.; Soleilhac, E.; Filhol, O. (2012). "Pharmacological Inhibition of LIM Kinase Stabilizes Microtubules and Inhibits Neoplastic Growth". Cancer Research. 72 (17): 4429–39. doi:10.1158/0008-5472.CAN-11-3342. PMID 22761334.
  2. ^ Pyridocarbazoles

External links edit

    January 01, 1970
    pyr1, liminib, organic, compound, composed, carbon, hydrogen, oxygen, nitrogen, that, inhibits, enzyme, kinase, names, preferred, iupac, name, dimethyl, dihydro, pyrido, carbazol, benzoate, other, names, liminib, identifiers, number, 83947, model, jsmol, inter. Pyr1 LIMINIB is an organic compound composed of carbon hydrogen oxygen and nitrogen that inhibits the enzyme LIM kinase Pyr1 Names Preferred IUPAC name 5 11 Dimethyl 1 oxo 2 6 dihydro 1H pyrido 4 3 b carbazol 9 yl benzoate Other names LIMINIB Identifiers CAS Number 83947 94 8 Y 3D model JSmol Interactive image ChemSpider 61709937 PubChem CID 13074411 UNII YL48YW74QQ Y InChI InChI 1S C24H18N2O3 c1 13 17 10 11 25 23 27 21 17 14 2 20 18 12 16 8 9 19 18 26 22 13 20 29 24 28 15 6 4 3 5 7 15 h3 12 26H 1 2H3 H 25 27 Key BPGBAEXPBQHBSV UHFFFAOYSA N SMILES O C C1 CC CC C1 OC C C2 CC3 C2NC4 C3C C C5C C CNC5 O C4C Properties Chemical formula C 24H 18N 2O 3 Molar mass 382 419 g mol 1 Except where otherwise noted data are given for materials in their standard state at 25 C 77 F 100 kPa Infobox references It was discovered by the Cure and Inserm Institute CNRS and CEA in the 2010s The studies in vitro and with animals 1 prove that this molecule has a completely new mechanism of action that could be used against chemotherapy resistant cells Pyr1 reversibly stabilizes microtubules blocks actin microfilament dynamics and inhibits cell motility in vitro These characteristics confer not only anticancer properties but also the capacity to prevent metastasis to the molecule Contents 1 Description and properties 2 Mechanism of action 3 Medical applications 4 References 5 External linksDescription and properties editPyr1 is classified as a small molecule that belongs to the group of pyridocarbazoles 2 Its small size gives it special properties as a light molecule it is a valuable tool for studying dynamic biological processes Therefore it is a key discovery in medical and biological investigation It is a high degree protein temporal controller as it is able to interact in a few minutes or even seconds with molecules such as LIMK1 Its reversibility enables it to quickly activate and inhibit itself making the molecule a specific inhibitor both in vitro and in cellulo Pyr1 can be described as a tetracyclic molecule with a simple structure Its few radicals are widely expanded along the benzene rings distinguishing a benzoyloxy group in the ninth carbon and two methyl radicals in carbon five and eleven There is also a ketone group in carbon one and two hydrogen radicals in carbons two and six Mechanism of action editPyr 1 is a cell permeable competitive inhibitor of Lim Kinase especially LIMK1 The latter is the enzyme that uses ATP to phosphorylate and inactivate the actin depolymerizing factor cofilin When cofilin is phosphorylated it regulates actin dynamics LIMK1 also depolymerizes microtubules nbsp Mechanism of action of LIMK1 In the presence of Pyr1 LIMK1 is inhibited which means that the phosphorylation of cofilin decreases which results in the blockage of the regulation of actin microfilaments dynamics and therefore the disorganization of microfilaments It also causes the stabilization of microtubules This inhibition is reversible In conclusion Pyr1 inhibits cell motility and controls actin dynamics and stabilizes microtubules These properties can be used in anticancer treatment nbsp Mechanism of action of Pyr1Medical applications editCancer metastasis consists in the fast and uncontrolled division of abnormal cells Microtubules have a key role in mitosis they generate the mitotic spindle assembly which allows chromosome segregation and the cell division Their stabilization leads to the inability of cells to reproduce or to their apoptosis That is why microtubule targeting agents are nowadays powerful anticancer drugs It also explains why tubulin is now considered as one of the most highly validated cancer targets These anticancer drugs have however some limitations due to side effects principally myelosuppression and neurotoxicity But the main inconvenience is that many cancers are or become resistant to these drugs Several strategies have been proposed for the development of more effective and less toxic anticancer drugs One of them is to use molecules that can induce the stabilization of microtubules and Pyr1 is one of them Pyr1 may be used in cancer treatment because its main target enzyme LIM kinase is a regulator of microtubule and actin dynamics Moreover it has been shown that Pyr1 is toxic for cancerous cell lines even the ones that are resistant to conventional microtubule targeting agents Furthermore the toxicity of Pyr1 has been studied in mice to evaluate whether it could really work as a chemotherapeutic agent The results show a complete survival of mice against xenografted tumors with no apparent toxicity as there was no loss of weight observed Therefore it has been concluded that Pyr1 has a good therapeutic efficacy preventing tumor growth at doses that are well tolerated by animals Bearing the previous points in mind Pyr1 may be used in addition or as an alternative to standard chemotherapy in drug resistant tumors References edit Prudent R Vassal Stermann E Nguyen C H Pillet C Martinez A Prunier C Barette C Soleilhac E Filhol O 2012 Pharmacological Inhibition of LIM Kinase Stabilizes Microtubules and Inhibits Neoplastic Growth Cancer Research 72 17 4429 39 doi 10 1158 0008 5472 CAN 11 3342 PMID 22761334 PyridocarbazolesExternal links editItineraire d une petite molecule aux proprietes anticancereuses prometteuses Retrieved from https en wikipedia org w index php title Pyr1 amp oldid 1105952756, wikipedia, wiki, book, books, library,

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