弗氏鹽

化合物

弗氏鹽是一種無機化合物,化學式 (K4[ON(SO3)2]2),有時寫作 (K2[NO(SO3)2])。它是一種亮黃棕色固體,但水溶液是亮紫色的。[1][2] 相關的鈉鹽亞硝基二磺酸鈉(簡稱NDS,化學式 Na2ON(SO3)2CAS號 29554-37-8)也被稱為弗氏鹽。[3]

弗氏鹽
IUPAC名
Potassium nitrosodisulfonate
別名 亞硝基二磺酸鉀
識別
CAS號 14293-70-0  checkY
PubChem 3032624
ChemSpider 2297553
SMILES
 
  • N([O])(S(=O)(=O)[O-])S(=O)(=O)[O-].[K+].[K+]
性質
化學式 K2NO(SO3)2
摩爾質量 268.33 (鉀鹽) g·mol⁻¹
危險性
警示術語 R:R14 R20/21/22
安全術語 S:S36
H-術語 H260, H302, H312, H332
P-術語 P223, P231+232, P280, P301+312, P302+352+312, P304+340+312
主要危害 有害 (Xn)
若非註明,所有數據均出自標準狀態(25 ℃,100 kPa)下。

應用

弗氏鹽作為一種長壽命的自由基,是電子自旋共振 (EPR) 的標準。其強烈的EPR譜線由三條等強度的線主導,間距約為 13 G(1.3 mT)。[4][5][6]

弗氏鹽可用於某些氧化反應,例如某些苯胺或苯酚的氧化。[7][8][9][10][11]它也允許肽和基於肽的水凝膠英語Hydrogel的聚合和交聯。[12][13]

它還可以用作研究中過氧自由基的模型,以研究各種天然產品中抗氧化作用的機制。[14]

製備

弗氏鹽可以由羥胺二磺酸開始製備而成。氧化它的共軛鹼可以得到紫色的雙陰離子

HON(SO3H)2 → [HON(SO3)2]2− + 2 H+
2 [HON(SO3)2]2− + PbO2 → 2 [ON(SO3)2]2− + PbO + H2O

羥胺二磺酸鹽則是由亞硝酸鹽亞硫酸氫鹽反應而成的。氧化反應通常是在低溫下進行的,可以通過化學方法或電解達成。[3][2]

其它製備方法:

HNO2 + 2 HSO
3
HON(SO
3
)2−
2
+ H2O
3 HON(SO
3
)2−
2
+ MnO
4
+ H+ → 3 ON(SO
3
)2−
2
+ MnO2 + 2 H2O
2 ON(SO
3
)2−
2
+ 4 K+ → K4[ON(SO3)2]2

歷史

弗氏鹽是在1845年由埃德蒙·弗雷米 (1814–1894)發現的。[15]

參考資料

  1. ^ Greenwood, Norman Neill; Earnshaw, Alan. Chemistry of the elements. 2016. ISBN 978-0-7506-3365-9. OCLC 1040112384 (英語). 
  2. ^ 2.0 2.1 Synthesis and Characterization of Potassium Nitrosodisulfonate, Frémy's Salt (PDF). tripod.com. [2021-12-03]. (原始內容 (PDF)存檔於2010-09-23). 
  3. ^ 3.0 3.1 Wehrli PA, Pigott F. Oxidation with the nitrosodisulfonate radical. I. Preparation and use of sodium nitrosodisulfonate: trimethyl-p-benzoquinone. Organic Syntheses. 1972, 52: 83. doi:10.15227/orgsyn.052.0083. 
  4. ^ Wertz JE, Bolton JR. Electron Spin Resonance: Elementary Theory and Practical Applications. New York: McGraw-Hill. 1972. ISBN 978-0-07-069454-5.  See page 463 for information on intensity measurements and page 86 for an EPR spectrum of Frémy's salt.
  5. ^ Colacicchi S, Carnicelli V, Gualtieri G, Di Giulio A. EPR study of Frémy's salt nitroxide reduction by ascorbic acid; influence of bulk pH values. Res. Chem. Intermed. 2000, 26 (9): 885–896. S2CID 98775951. doi:10.1163/156856700X00372. 
  6. ^ Zielonka J, Zhao H, Xu Y, Kalyanaraman B. Mechanistic similarities between oxidation of hydroethidine by Frémy's salt and superoxide: stopped-flow optical and EPR studies. Free Radical Biology & Medicine. October 2005, 39 (7): 853–863. PMID 16140206. doi:10.1016/j.freeradbiomed.2005.05.001. 
  7. ^ Zimmer H, Lankin DC, Horgan SW. Oxidations with potassium nitrosodisulfonate (Frémy's radical). Teuber reaction.. Chemical Reviews. 1971, 71 (2): 229–246. doi:10.1021/cr60270a005. 
  8. ^ Islam I, Skibo EB, Dorr RT, Alberts DS. Structure-activity studies of antitumor agents based on pyrrolo[1,2-a]benzimidazoles: new reductive alkylating DNA cleaving agents. Journal of Medicinal Chemistry. October 1991, 34 (10): 2954–2961. PMID 1920349. doi:10.1021/jm00114a003. 
  9. ^ Teuber HJ, Benz S. Reaktionen mit Nitrosodisulfonat, XXXVI. Chinolin-chinone-(5.6) aus 5-Hydroxy-chinolinen. Chem. Ber. 1967, 100 (9): 2918–2929. doi:10.1002/cber.19671000916 (德語). [失效連結]
  10. ^ Teuber HJ. Use of dipotassium nitrosodisulfonate (Frémy's salt): 4,5-dimethyl-o-benzoquinone. Org. Synth. 1972, 52: 88. doi:10.15227/orgsyn.052.0088. 
  11. ^ Xue W, Warshawsky D, Rance M, Jayasimhulu K. A metabolic activation mechanism of 7H-dibenzo[c,g]carbozole via o-quinone. Part 1: synthesis of 7H-dibenzo[c,g]carbozole-3,4-dione and reactions with nucleophiles. Polycyclic Aromatic Compounds. 2002, 22 (3–4): 295–300. S2CID 95507636. doi:10.1080/10406630290026957. 
  12. ^ Wilchek M, Miron T. Mussel-inspired new approach for polymerization and cross-linking of peptides and proteins containing tyrosines by Frémy's salt oxidation. Bioconjugate Chemistry. March 2015, 26 (3): 502–510. PMID 25692389. doi:10.1021/bc5006152. 
  13. ^ Fichman G, Schneider JP. Utilizing Frémy's Salt to Increase the Mechanical Rigidity of Supramolecular Peptide-Based Gel Networks. Frontiers in Bioengineering and Biotechnology. 2021, 8: 594258. PMC 7813677 . PMID 33469530. doi:10.3389/fbioe.2020.594258  (英語). 
  14. ^ Liu ZL, Han ZX, Chen P, Liu YC. Stopped-flow ESR study on the reactivity of vitamin E, vitamin C and its lipophilic derivatives towards Frémy's salt in micellar systems. Chemistry and Physics of Lipids. November 1990, 56 (1): 73–80. PMID 1965427. doi:10.1016/0009-3084(90)90090-E. 
  15. ^ 參見:

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