Chemistry:Valinomycin

Valinomycin
Names
	IUPAC name cyclo[N-oxa-D-alanyl-D-valyl-N-oxa-L-valyl-D-valyl-N-oxa-D-alanyl-D-valyl-N-oxa-L-valyl-L-valyl-N-oxa-L-alanyl-L-valyl-N-oxa-L-valyl-L-valyl]
Identifiers
CAS Number	2001-95-8 ;
3D model (JSmol)	: Interactive image;
ChEBI	CHEBI:28545 ;
ChEMBL	ChEMBL223643 ;
ChemSpider	21493802 ;
DrugBank	DB14057;
EC Number	217-896-6;
PubChem CID	3000706;
UNII	N561YS75MN ;
UN number	2811 2588
	InChI InChI=1S/C54H90N6O18/c1-22(2)34-49(67)73-31(19)43(61)55-38(26(9)10)53(71)77-41(29(15)16)47(65)59-36(24(5)6)51(69)75-33(21)45(63)57-39(27(11)12)54(72)78-42(30(17)18)48(66)60-35(23(3)4)50(68)74-32(20)44(62)56-37(25(7)8)52(70)76-40(28(13)14)46(64)58-34/h22-42H,1-21H3,(H,55,61)(H,56,62)(H,57,63)(H,58,64)(H,59,65)(H,60,66)/t31-,32-,33-,34+,35+,36+,37-,38-,39-,40+,41+,42+/m0/s1 Key: FCFNRCROJUBPLU-DNDCDFAISA-N ; InChI=1S/C54H90N6O18/c1-22(2)34-49(67)73-31(19)43(61)55-38(26(9)10)53(71)77-41(29(15)16)47(65)59-36(24(5)6)51(69)75-33(21)45(63)57-39(27(11)12)54(72)78-42(30(17)18)48(66)60-35(23(3)4)50(68)74-32(20)44(62)56-37(25(7)8)52(70)76-40(28(13)14)46(64)58-34/h22-42H,1-21H3,(H,55,61)(H,56,62)(H,57,63)(H,58,64)(H,59,65)(H,60,66)/t31-,32-,33+,34-,35+,36+,37-,38-,39+,40+,41+,42+/m1/s1 Key: FCFNRCROJUBPLU-DNDCDFAIBE;
	SMILES : C[C@@H]1C(=O)N[C@@H](C(=O)O[C@H](C(=O)N[C@@H](C(=O)O[C@@H](C(=O)N[C@@H](C(=O)O[C@H](C(=O)N[C@H](C(=O)O[C@H](C(=O)N[C@H](C(=O)O[C@H](C(=O)N[C@H](C(=O)O1)C(C)C)C(C)C)C(C)C)C)C(C)C)C(C)C)C(C)C)C)C(C)C)C(C)C)C(C)C;
Properties
Chemical formula	C54H90N6O18
Molar mass	1111.32 g/mol
Appearance	White solid
Melting point	190 °C (374 °F; 463 K)
Solubility	Methanol, ethanol, ethyl acetate, petrol-ether, dichloromethane
UV-vis (λmax)	220 nm
Hazards
Main hazards	Neurotoxicant
GHS pictograms
GHS Signal word	Danger
GHS hazard statements	H300, H310
GHS precautionary statements	P262, P264, P270, P280, P301+310, P302+350, P310, P321, P322, P330, P361, P363, P405, P501
	Lethal dose or concentration (LD, LC):
LD50 (median dose)	4 mg/kg (oral, rat)
	Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa).
	verify (what is ?)
	Infobox references

The printable version is no longer supported and may have rendering errors. Please update your browser bookmarks and please use the default browser print function instead.

Valinomycin is a naturally occurring dodecadepsipeptide used in the transport of potassium and as an antibiotic. Valinomycin is obtained from the cells of several Streptomyces species, S. fulvissimus being a notable one.

It is a member of the group of natural neutral ionophores because it does not have a residual charge. It consists of enantiomers D- and L-valine (Val), D-alpha-hydroxyisovaleric acid, and L-lactic acid. Structures are alternately bound via amide and ester bridges. Valinomycin is highly selective for potassium ions over sodium ions within the cell membrane.^[2] It functions as a potassium-specific transporter and facilitates the movement of potassium ions through lipid membranes "down" the electrochemical potential gradient.^[3] The stability constant K for the potassium-valinomycin complex is nearly 100,000 times larger than that of the sodium-valinomycin complex.^[4] This difference is important for maintaining the selectivity of valinomycin for the transport of potassium ions (and not sodium ions) in biological systems.

It is classified as an extremely hazardous substance in the United States as defined in Section 302 of the U.S. Emergency Planning and Community Right-to-Know Act (42 U.S.C. 11002), and is subject to strict reporting requirements by facilities which produce, store, or use it in significant quantities.^[5]

Structure

Valinomycin is a dodecadepsipeptide, that is, it is made of twelve alternating amino acids and esters to form a macrocyclic molecule. The twelve carbonyl groups are essential for the binding of metal ions, and also for solvation in polar solvents. The isopropyl and methyl groups are responsible for solvation in nonpolar solvents. ^[6] Along with its shape and size this molecular duality is the main reason for its binding properties. K ions must give up their water of hydration to pass through the pore. K⁺ ions are octahedrally coordinated in a square bipyramidal geometry by 6 carbonyl bonds from Val. In this space of 1.33 Angstrom, Na⁺ with its 0.95 Angstrom radius, is significantly smaller than the channel, meaning that Na⁺ cannot form ionic bonds with the amino acids of the pore at equivalent energy as those it gives up with the water molecules. This leads to a 10,000x selectivity for K⁺ ions over Na⁺. For polar solvents, valinomycin will mainly expose the carbonyls to the solvent and in nonpolar solvents the isopropyl groups are located predominantly on the exterior of the molecule. This conformation changes when valinomycin is bound to a potassium ion. The molecule is "locked" into a conformation with the isopropyl groups on the exterior [Citation Needed]. It is not actually locked into configuration because the size of the molecule makes it highly flexible, but the potassium ion gives some degree of coordination to the macromolecule.

Applications

Valinomycin was recently reported to be the most potent agent against severe acute respiratory-syndrome coronavirus (SARS-CoV) in infected Vero E6 cells.^[7]

Valinomycin acts as a nonmetallic isoforming agent in potassium selective electrodes.^[8]^[9]

This ionophore is used to study membrane vesicles, where it may be selectively applied by experimental design to reduce or eliminate the electrochemical gradient across a membrane.^{[citation needed]}

References

↑ ^1.0 ^1.1 "ChemIDplus - 2001-95-8 - FCFNRCROJUBPLU-DNDCDFAISA-N - Valinomycin - Similar structures search, synonyms, formulas, resource links, and other chemical information". U.S. National Library of Medicine. https://chem.nlm.nih.gov/chemidplus/rn/2001-95-8.
↑ Lars, Rose; Jenkins ATA (2007). "The effect of the ionophore valinomycin on biomimetic solid supported lipid DPPTE/EPC membranes". Bioelectrochemistry 70 (2): 387–393. doi:10.1016/j.bioelechem.2006.05.009. PMID 16875886.
↑ Cammann K (1985). "Ion-selective bulk membranes as models". Top. Curr. Chem.. Topics in Current Chemistry 128: 219–258. doi:10.1007/3-540-15136-2_8. ISBN 978-3-540-15136-4.
↑ Rose, M.C.; Henkens, R.W. (1974). "Stability of sodium and potassium complexes of valinomycin". Biochimica et Biophysica Acta (BBA) - General Subjects 372 (2): 426–435. doi:10.1016/0304-4165(74)90204-9.
↑ 40 C.F.R.: Appendix A to Part 355—The List of Extremely Hazardous Substances and Their Threshold Planning Quantities (July 1, 2008 ed.). Government Printing Office. http://edocket.access.gpo.gov/cfr_2008/julqtr/pdf/40cfr355AppA.pdf. Retrieved October 29, 2011.
↑ "The electroanalytical response of the bilayer lipid membrane to valinomycin: membrane cholesterol content". Anal. Chim. Acta 141: 33–47. 1982. doi:10.1016/S0003-2670(01)95308-5.
↑ Zhang, Dong; Ma, Zhi; Chen, Hanchi; Lu, Yuele; Chen, Xiaolong (October 2020). "Valinomycin as a potential antiviral agent against coronaviruses: A review". Biomedical Journal 43 (5): 414–423. doi:10.1016/j.bj.2020.08.006. ISSN 2319-4170. PMID 33012699.
↑ "Loss of mitochondrial membrane potential is associated with increase in mitochondrial volume: physiological role in neurones". J. Cell. Physiol. 206 (2): 347–353. 2006. doi:10.1002/jcp.20476. PMID 16110491.
↑ Potassium ionophore Bulletin

External links

Chemical Safety Regulations from New Jersey Department of Health.
Health information on Scorecard.
Valinomycin from Fermentek.
Valinomycin in the Pesticide Properties DataBase (PPDB)

0.00

(0 votes)

Original source: https://en.wikipedia.org/wiki/Valinomycin. Read more

[chemidplus-1] 1.0 ^1.1 "ChemIDplus - 2001-95-8 - FCFNRCROJUBPLU-DNDCDFAISA-N - Valinomycin - Similar structures search, synonyms, formulas, resource links, and other chemical information". U.S. National Library of Medicine. https://chem.nlm.nih.gov/chemidplus/rn/2001-95-8.

[2] Lars, Rose; Jenkins ATA (2007). "The effect of the ionophore valinomycin on biomimetic solid supported lipid DPPTE/EPC membranes". Bioelectrochemistry 70 (2): 387–393. doi:10.1016/j.bioelechem.2006.05.009. PMID 16875886.

[3] Cammann K (1985). "Ion-selective bulk membranes as models". Top. Curr. Chem.. Topics in Current Chemistry 128: 219–258. doi:10.1007/3-540-15136-2_8. ISBN 978-3-540-15136-4.

[4] Rose, M.C.; Henkens, R.W. (1974). "Stability of sodium and potassium complexes of valinomycin". Biochimica et Biophysica Acta (BBA) - General Subjects 372 (2): 426–435. doi:10.1016/0304-4165(74)90204-9.

[gov-right-know-5] 40 C.F.R.: Appendix A to Part 355—The List of Extremely Hazardous Substances and Their Threshold Planning Quantities (July 1, 2008 ed.). Government Printing Office. http://edocket.access.gpo.gov/cfr_2008/julqtr/pdf/40cfr355AppA.pdf. Retrieved October 29, 2011.

[6] "The electroanalytical response of the bilayer lipid membrane to valinomycin: membrane cholesterol content". Anal. Chim. Acta 141: 33–47. 1982. doi:10.1016/S0003-2670(01)95308-5.

[7] Zhang, Dong; Ma, Zhi; Chen, Hanchi; Lu, Yuele; Chen, Xiaolong (October 2020). "Valinomycin as a potential antiviral agent against coronaviruses: A review". Biomedical Journal 43 (5): 414–423. doi:10.1016/j.bj.2020.08.006. ISSN 2319-4170. PMID 33012699.

[8] "Loss of mitochondrial membrane potential is associated with increase in mitochondrial volume: physiological role in neurones". J. Cell. Physiol. 206 (2): 347–353. 2006. doi:10.1002/jcp.20476. PMID 16110491.

[9] Potassium ionophore Bulletin

[1]

[2]

[3]

[4]

[5]

[6]

[7]

[8]

[9]

Anonymous

Search

Chemistry:Valinomycin

Namespaces

More

Page actions

Contents

Structure

Applications

References

External links

Navigation

Navigation

Help

Translate

Wiki tools

Wiki tools

Anonymous

Search

Chemistry:Valinomycin

Structure

Applications

References

External links

Navigation

Wiki tools

Page tools

Other projects

Categories