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Rebecca Abergel

Rebecca Abergel is a French inorganic chemist who specializes in the coordination chemistry between lanthanide and actinide complexes. Alongside the effects of heavy element exposure and contamination on different biological systems. Abergel is currently a faculty scientist and heavy element chemistry group leader at the chemical sciences division of Lawrence Berkeley National Laboratory in Berkeley, California. She is also assistant professor of nuclear engineering at University of California, Berkeley.[1][2]

Rebecca Abergel
Alma materÉcole Normale Supérieure (B.Sc.) (2002)
University of California, Berkeley (Ph.D) (2006)
Scientific career
FieldsCoordination Chemistry, Environmental Chemistry
InstitutionsUniversity of California, Berkeley
Doctoral advisorKen Raymond
Websiteabergel.lbl.gov

Early life and education edit

Abergel grew up near Paris, France, where she received her undergraduate degree in chemistry from École Normale Supérieure in 2002. While an undergraduate, she received a scholarship to work under Prof. John Arnold, an inorganic chemist at the University of California, Berkeley.[3]

She then pursued graduate studies at UC Berkeley, where she worked with Prof. Ken Raymond. For her doctoral work, she synthesised and characterised siderophore analogs to investigate how bacteria transport iron and to develop new iron chelating agents.[3][4][5][6][7][8] Abergel graduated in 2006 with her Ph.D. in Chemistry.[2]

Abergel was a joint postdoctoral researcher between the UC Berkeley Department of Chemistry and the group of Prof. Roland Strong at the Fred Hutchinson Cancer Research Center. Here she investigated how siderocalin binds to siderophores from bacteria such as Bacillus anthracis, for the development of new antibiotics.[9][10][11]

Abergel joined Berkeley Lab in 2009; she received a Young Investigator Award from the Cooley's Anemia Foundation in 2009, a Junior Faculty Travel Award from the Radiation Research Society in 2013, and a Director's Award for Exceptional Scientific Achievement from Berkeley Lab in 2013.

Research interests edit

Abergel's BioActinide Research group conducts a variety of different experiments in the field of coordination chemistry, analytical chemistry, photophysics, biological chemistry, health physics, pharmacology, molecular biology, and cell biology. More specifically, her recent interests have focused on the coordination behavior of lanthanides and actinides.[12] Her group is especially active in developing healing methods to treat people who have been exposed to radionuclides or atoms that contain excess nuclear charge. In recent work by the BioActinide Research group, different actinide chelating agents have been synthesised which could be used to selectively bind radionuclides in the human body in order to safely remove them.[13]

 
Figure 1 - DTPA

Currently, the only drug approved by the Food and Drug Administration to treat radionuclide contamination is diethylenetriaminepentaacetic acid (DTPA) (Figure 1). DTPA has shown some promise in treating plutonium poisoning, but this treatment is specific only to plutonium.[14] Furthermore, DTPA must be administered intravenously, which is an issue due to the extremely time-sensitive nature of radiation poisoning. In the quest of finding a more versatile and easily administered treatment for radiation poisoning, Abergel sees potential in developing new classes of therapeutics.

The agent under investigation is an octadentate ligand consisting of four cross-linked dipicolinic acid components (Figure 2). This molecule is unique in having the potential for oral consumption in humans.[15] It would function by coordinating as a chelating ligand with toxic actinides in the body before they can cause significant damage. In theory, once the chelating ligands have bound to the actinides, the heavy metal complexes can exit the body naturally by urination.[14]

 
Figure 2 - 3,4,3-LI(1,2-HOPO)

Due to its octadentate structure, the chelator of interest exhibits higher affinity for lanthanides in vivo than DTPA. Therefore, it has demonstrated better radionuclide decorporation in living systems.[16] The ligand has shown favorable selectivity for plutonium, americium, uranium, and neptunium decorporation (with no observed toxicity in either in vitro tests on human tissue or in vivo experiments on rodent models), which is also an improvement over the currently accepted DTPA.[17] Finally, in a separate study, Abergel evaluated the purity of this molecule for use as a drug, ultimately bringing this effort closer to the development of a deployable treatment solution.[18]

 
Figure 3 - 5-LIO(Me-3,2-HOPO)

An additional research project by Abergel's group involved testing the effectiveness of other analogs containing dipicolinic acid in eliminating plutonium (Figure 3). Results showed that both of the compounds were successful in removing plutonium over a seven-day period in mice.[19] Overall, this work, along with further studies focusing on lanthanide and actinide chelation, has important implications for medicinal and environmental chemistry.[20][21]

Awards and fellowships edit

  • Directors Award for Exceptional Scientific Achievement (2013), Lawrence Berkeley National Laboratory, US
  • Junior Faculty NCRP Award (2013), Radiation Research Society, US
  • Young Investor Research Fellowship (2009–2010), Cooley's Anemia Foundation, New York, NY, US
  • European Commission Marie Curie Actions Scholarship (2004), European School of Haematology, France
  • Université Pierre et Marie Curie Annual Fellowship (2002), French Conseil Régional d’Ile de France, France

References edit

  1. ^ "People". abergel.lbl.gov. Retrieved 2021-05-18.
  2. ^ a b "Rebecca Abergel - Chemical Sciences Division Chemical Sciences Division". commons.lbl.gov. Retrieved 2021-05-18.
  3. ^ a b "Women @ The Lab - Rebecca Abergel, Ph.D." sites.google.com. Retrieved 2021-05-18.
  4. ^ Abergel, Rebecca J.; Raymond, Kenneth N. (2006-05-01). "Synthesis and Thermodynamic Evaluation of Mixed Hexadentate Linear Iron Chelators Containing Hydroxypyridinone and Terephthalamide Units1". Inorganic Chemistry. 45 (9): 3622–3631. doi:10.1021/ic052111a. ISSN 0020-1669. PMC 3685440. PMID 16634594.
  5. ^ Abergel, Rebecca J.; Warner, Jeffrey A.; Shuh, David K.; Raymond, Kenneth N. (2006-07-01). "Enterobactin Protonation and Iron Release: Structural Characterization of the Salicylate Coordination Shift in Ferric Enterobactin1". Journal of the American Chemical Society. 128 (27): 8920–8931. doi:10.1021/ja062046j. ISSN 0002-7863. PMC 3188320. PMID 16819888.
  6. ^ Abergel, Rebecca J.; Raymond, Kenneth N. (2008-02-01). "Terephthalamide-containing ligands: fast removal of iron from transferrin". Journal of Biological Inorganic Chemistry. 13 (2): 229–240. doi:10.1007/s00775-007-0314-y. ISSN 1432-1327. PMID 17990009. S2CID 20706644.
  7. ^ Abergel, Rebecca J.; Zawadzka, Anna M.; Raymond, Kenneth N. (2008-02-01). "Petrobactin-Mediated Iron Transport in Pathogenic Bacteria: Coordination Chemistry of an Unusual 3,4-Catecholate/Citrate Siderophore". Journal of the American Chemical Society. 130 (7): 2124–2125. doi:10.1021/ja077202g. ISSN 0002-7863. PMID 18220393.
  8. ^ Abergel, Rebecca J.; Zawadzka, Anna M.; Hoette, Trisha M.; Raymond, Kenneth N. (2009-09-09). "Enzymatic Hydrolysis of Trilactone Siderophores: Where Chiral Recognition Occurs in Enterobactin and Bacillibactin Iron Transport". Journal of the American Chemical Society. 131 (35): 12682–12692. doi:10.1021/ja903051q. ISSN 0002-7863. PMC 2782669. PMID 19673474.
  9. ^ Abergel, Rebecca J.; Moore, Evan G.; Strong, Roland K.; Raymond, Kenneth N. (2006-08-01). "Microbial Evasion of the Immune System: Structural Modifications of Enterobactin Impair Siderocalin Recognition". Journal of the American Chemical Society. 128 (34): 10998–10999. doi:10.1021/ja062476+. ISSN 0002-7863. PMC 3188317. PMID 16925397.
  10. ^ Abergel, Rebecca J.; Wilson, Melissa K.; Arceneaux, Jean E. L.; Hoette, Trisha M.; Strong, Roland K.; Byers, B. Rowe; Raymond, Kenneth N. (2006-12-05). "Anthrax pathogen evades the mammalian immune system through stealth siderophore production". Proceedings of the National Academy of Sciences. 103 (49): 18499–18503. Bibcode:2006PNAS..10318499A. doi:10.1073/pnas.0607055103. ISSN 0027-8424. PMC 1693691. PMID 17132740.
  11. ^ Abergel, Rebecca J.; Clifton, Matthew C.; Pizarro, Juan C.; Warner, Jeffrey A.; Shuh, David K.; Strong, Roland K.; Raymond, Kenneth N. (2008-08-27). "The Siderocalin/Enterobactin Interaction: A Link between Mammalian Immunity and Bacterial Iron Transport1". Journal of the American Chemical Society. 130 (34): 11524–11534. doi:10.1021/ja803524w. ISSN 0002-7863. PMC 3188318. PMID 18680288.
  12. ^ "Women @ The Lab". 2013.
  13. ^ Jarvis, Erin E.; An, Dahlia D.; Kullgren, Birgitta; Abergel, Rebecca J. (2012). "Significance of Single Variables in Defining Adequate Animal Models to Assess the Efficacy of New Radionuclide Decorporation Agents: Using the Contamination Dose as an Example". Drug Development Research. 73 (5): 281–289. doi:10.1002/ddr.21020. S2CID 82740785.
  14. ^ a b "Rebecca Abergel".
  15. ^ Choi, Taylor A.; Furimsky, Anna M.; Swezey, Robert; Bunin, Deborah I.; Byrge, Patricia; Iyer, Lalitha V.; Chang, Polly Y.; Abergel, Rebecca J. (2015). "In Vitro Metabolism and Stability of the Actinide Chelating Agent 3,4,3-LI(1,2-HOPO)". Journal of Pharmaceutical Sciences. 104 (5): 1832–1838. doi:10.1002/jps.24394. PMC 4390475. PMID 25727482.
  16. ^ Sturzbecher-Hoehne, Manuel; Ng Pak Leung, Clara; d'Aléo, Anthony; Kullgren, Birgitta; Prigent, Anne-Laure; Shuh, David K.; Raymond, Kenneth N.; Abergel, Rebecca J. (2011). "3,4,3-LI(1,2-HOPO): In Vitro Formation of Highly Stable Lanthanide Complexes Translates into Efficacious In Vivo Europium Decorporation" (PDF). Dalton Transactions. 40 (33): 8340–6. doi:10.1039/c1dt10840a. OSTI 1051843. PMID 21766096. S2CID 33758070.
  17. ^ Abergel, R. J.; Durbin, P. W.; Kullgren, B.; Ebbe, S. N.; Xu, J.; Chang, P. Y.; Bunin, D. I.; Blakely, E. A.; Bjornstad, K. A.; Rosen, C. J.; Shuh, D. K.; Raymond, K. N. (2010). "Biomimetic Actinide Chelators: An Update on the Preclinical Development of the Orally Active Hydroxypyridonate Decorporation Agents 3,4,3-LI(1,2-HOPO) and 5-LIO(Me-3,2-HOPO)". Health Phys. 99 (3): 401–407. doi:10.1097/HP.0b013e3181c21273. PMC 2921233. PMID 20699704.
  18. ^ Panyala, Nagender R.; Sturzbecher-Hoehne, Manuel; Abergel, Rebecca J. (2014). "Identification of process related trace level impurities in the actinide decorporation agent 3,4,3-LI(1,2-HOPO): Nozzle–skimmer fragmentation via ESI LC–QTOFMS". Journal of Pharmaceutical and Biomedical Analysis. 100: 157–166. doi:10.1016/j.jpba.2014.08.004. PMC 4179986. PMID 25165012.
  19. ^ An, Dahlia D.; Kullgren, Birgitta; Jarvis, Erin E.; Abergel, Rebecca J. (2017). "From early prophylaxis to delayed treatment: Establishing the plutonium decorporation activity window of hydroxypyridinonate chelating agents". Chemico-Biological Interactions. 267: 80–88. doi:10.1016/j.cbi.2016.03.034. PMC 5045775. PMID 27038878.
  20. ^ Abergel, Rebecca J.; Ansoborlo, Eric (2016-04-22). "Curious curium". Nature Chemistry. 8 (5): 516. Bibcode:2016NatCh...8..516A. doi:10.1038/nchem.2512. OSTI 1458477. PMID 27102687. S2CID 12473941.
  21. ^ Deblonde, Gauthier J-P.; Sturzbecher-Hoehne, Manuel; Abergel, Rebecca J. (2013). "Solution Thermodynamic Stability of Complexes Formed with the Octadentate Hydroxypyridinonate Ligand 3,4,3-LI(1,2-HOPO): A Critical Feature for Efficient Chelation of Lanthanide(IV) and Actinide(IV) Ions". Inorganic Chemistry. 52 (15): 8805–8811. doi:10.1021/ic4010246. PMC 3771511. PMID 23855806.

rebecca, abergel, this, article, multiple, issues, please, help, improve, discuss, these, issues, talk, page, learn, when, remove, these, template, messages, this, article, contain, excessive, amount, intricate, detail, that, interest, only, particular, audien. This article has multiple issues Please help improve it or discuss these issues on the talk page Learn how and when to remove these template messages This article may contain an excessive amount of intricate detail that may interest only a particular audience Please help by spinning off or relocating any relevant information and removing excessive detail that may be against Wikipedia s inclusion policy January 2018 Learn how and when to remove this template message This article may be too technical for most readers to understand Please help improve it to make it understandable to non experts without removing the technical details January 2018 Learn how and when to remove this template message Learn how and when to remove this template message Rebecca Abergel is a French inorganic chemist who specializes in the coordination chemistry between lanthanide and actinide complexes Alongside the effects of heavy element exposure and contamination on different biological systems Abergel is currently a faculty scientist and heavy element chemistry group leader at the chemical sciences division of Lawrence Berkeley National Laboratory in Berkeley California She is also assistant professor of nuclear engineering at University of California Berkeley 1 2 Rebecca AbergelAlma materEcole Normale Superieure B Sc 2002 University of California Berkeley Ph D 2006 Scientific careerFieldsCoordination Chemistry Environmental ChemistryInstitutionsUniversity of California BerkeleyDoctoral advisorKen RaymondWebsiteabergel wbr lbl wbr gov Contents 1 Early life and education 2 Research interests 3 Awards and fellowships 4 ReferencesEarly life and education editAbergel grew up near Paris France where she received her undergraduate degree in chemistry from Ecole Normale Superieure in 2002 While an undergraduate she received a scholarship to work under Prof John Arnold an inorganic chemist at the University of California Berkeley 3 She then pursued graduate studies at UC Berkeley where she worked with Prof Ken Raymond For her doctoral work she synthesised and characterised siderophore analogs to investigate how bacteria transport iron and to develop new iron chelating agents 3 4 5 6 7 8 Abergel graduated in 2006 with her Ph D in Chemistry 2 Abergel was a joint postdoctoral researcher between the UC Berkeley Department of Chemistry and the group of Prof Roland Strong at the Fred Hutchinson Cancer Research Center Here she investigated how siderocalin binds to siderophores from bacteria such as Bacillus anthracis for the development of new antibiotics 9 10 11 Abergel joined Berkeley Lab in 2009 she received a Young Investigator Award from the Cooley s Anemia Foundation in 2009 a Junior Faculty Travel Award from the Radiation Research Society in 2013 and a Director s Award for Exceptional Scientific Achievement from Berkeley Lab in 2013 Research interests editAbergel s BioActinide Research group conducts a variety of different experiments in the field of coordination chemistry analytical chemistry photophysics biological chemistry health physics pharmacology molecular biology and cell biology More specifically her recent interests have focused on the coordination behavior of lanthanides and actinides 12 Her group is especially active in developing healing methods to treat people who have been exposed to radionuclides or atoms that contain excess nuclear charge In recent work by the BioActinide Research group different actinide chelating agents have been synthesised which could be used to selectively bind radionuclides in the human body in order to safely remove them 13 nbsp Figure 1 DTPACurrently the only drug approved by the Food and Drug Administration to treat radionuclide contamination is diethylenetriaminepentaacetic acid DTPA Figure 1 DTPA has shown some promise in treating plutonium poisoning but this treatment is specific only to plutonium 14 Furthermore DTPA must be administered intravenously which is an issue due to the extremely time sensitive nature of radiation poisoning In the quest of finding a more versatile and easily administered treatment for radiation poisoning Abergel sees potential in developing new classes of therapeutics The agent under investigation is an octadentate ligand consisting of four cross linked dipicolinic acid components Figure 2 This molecule is unique in having the potential for oral consumption in humans 15 It would function by coordinating as a chelating ligand with toxic actinides in the body before they can cause significant damage In theory once the chelating ligands have bound to the actinides the heavy metal complexes can exit the body naturally by urination 14 nbsp Figure 2 3 4 3 LI 1 2 HOPO Due to its octadentate structure the chelator of interest exhibits higher affinity for lanthanides in vivo than DTPA Therefore it has demonstrated better radionuclide decorporation in living systems 16 The ligand has shown favorable selectivity for plutonium americium uranium and neptunium decorporation with no observed toxicity in either in vitro tests on human tissue or in vivo experiments on rodent models which is also an improvement over the currently accepted DTPA 17 Finally in a separate study Abergel evaluated the purity of this molecule for use as a drug ultimately bringing this effort closer to the development of a deployable treatment solution 18 nbsp Figure 3 5 LIO Me 3 2 HOPO An additional research project by Abergel s group involved testing the effectiveness of other analogs containing dipicolinic acid in eliminating plutonium Figure 3 Results showed that both of the compounds were successful in removing plutonium over a seven day period in mice 19 Overall this work along with further studies focusing on lanthanide and actinide chelation has important implications for medicinal and environmental chemistry 20 21 Awards and fellowships editDirectors Award for Exceptional Scientific Achievement 2013 Lawrence Berkeley National Laboratory US Junior Faculty NCRP Award 2013 Radiation Research Society US Young Investor Research Fellowship 2009 2010 Cooley s Anemia Foundation New York NY US European Commission Marie Curie Actions Scholarship 2004 European School of Haematology France Universite Pierre et Marie Curie Annual Fellowship 2002 French Conseil Regional d Ile de France FranceReferences edit People abergel lbl gov Retrieved 2021 05 18 a b Rebecca Abergel Chemical Sciences Division Chemical Sciences Division commons lbl gov Retrieved 2021 05 18 a b Women The Lab Rebecca Abergel Ph D sites google com Retrieved 2021 05 18 Abergel Rebecca J Raymond Kenneth N 2006 05 01 Synthesis and Thermodynamic Evaluation of Mixed Hexadentate Linear Iron Chelators Containing Hydroxypyridinone and Terephthalamide Units1 Inorganic Chemistry 45 9 3622 3631 doi 10 1021 ic052111a ISSN 0020 1669 PMC 3685440 PMID 16634594 Abergel Rebecca J Warner Jeffrey A Shuh David K Raymond Kenneth N 2006 07 01 Enterobactin Protonation and Iron Release Structural Characterization of the Salicylate Coordination Shift in Ferric Enterobactin1 Journal of the American Chemical Society 128 27 8920 8931 doi 10 1021 ja062046j ISSN 0002 7863 PMC 3188320 PMID 16819888 Abergel Rebecca J Raymond Kenneth N 2008 02 01 Terephthalamide containing ligands fast removal of iron from transferrin Journal of Biological Inorganic Chemistry 13 2 229 240 doi 10 1007 s00775 007 0314 y ISSN 1432 1327 PMID 17990009 S2CID 20706644 Abergel Rebecca J Zawadzka Anna M Raymond Kenneth N 2008 02 01 Petrobactin Mediated Iron Transport in Pathogenic Bacteria Coordination Chemistry of an Unusual 3 4 Catecholate Citrate Siderophore Journal of the American Chemical Society 130 7 2124 2125 doi 10 1021 ja077202g ISSN 0002 7863 PMID 18220393 Abergel Rebecca J Zawadzka Anna M Hoette Trisha M Raymond Kenneth N 2009 09 09 Enzymatic Hydrolysis of Trilactone Siderophores Where Chiral Recognition Occurs in Enterobactin and Bacillibactin Iron Transport Journal of the American Chemical Society 131 35 12682 12692 doi 10 1021 ja903051q ISSN 0002 7863 PMC 2782669 PMID 19673474 Abergel Rebecca J Moore Evan G Strong Roland K Raymond Kenneth N 2006 08 01 Microbial Evasion of the Immune System Structural Modifications of Enterobactin Impair Siderocalin Recognition Journal of the American Chemical Society 128 34 10998 10999 doi 10 1021 ja062476 ISSN 0002 7863 PMC 3188317 PMID 16925397 Abergel Rebecca J Wilson Melissa K Arceneaux Jean E L Hoette Trisha M Strong Roland K Byers B Rowe Raymond Kenneth N 2006 12 05 Anthrax pathogen evades the mammalian immune system through stealth siderophore production Proceedings of the National Academy of Sciences 103 49 18499 18503 Bibcode 2006PNAS 10318499A doi 10 1073 pnas 0607055103 ISSN 0027 8424 PMC 1693691 PMID 17132740 Abergel Rebecca J Clifton Matthew C Pizarro Juan C Warner Jeffrey A Shuh David K Strong Roland K Raymond Kenneth N 2008 08 27 The Siderocalin Enterobactin Interaction A Link between Mammalian Immunity and Bacterial Iron Transport1 Journal of the American Chemical Society 130 34 11524 11534 doi 10 1021 ja803524w ISSN 0002 7863 PMC 3188318 PMID 18680288 Women The Lab 2013 Jarvis Erin E An Dahlia D Kullgren Birgitta Abergel Rebecca J 2012 Significance of Single Variables in Defining Adequate Animal Models to Assess the Efficacy of New Radionuclide Decorporation Agents Using the Contamination Dose as an Example Drug Development Research 73 5 281 289 doi 10 1002 ddr 21020 S2CID 82740785 a b Rebecca Abergel Choi Taylor A Furimsky Anna M Swezey Robert Bunin Deborah I Byrge Patricia Iyer Lalitha V Chang Polly Y Abergel Rebecca J 2015 In Vitro Metabolism and Stability of the Actinide Chelating Agent 3 4 3 LI 1 2 HOPO Journal of Pharmaceutical Sciences 104 5 1832 1838 doi 10 1002 jps 24394 PMC 4390475 PMID 25727482 Sturzbecher Hoehne Manuel Ng Pak Leung Clara d Aleo Anthony Kullgren Birgitta Prigent Anne Laure Shuh David K Raymond Kenneth N Abergel Rebecca J 2011 3 4 3 LI 1 2 HOPO In Vitro Formation of Highly Stable Lanthanide Complexes Translates into Efficacious In Vivo Europium Decorporation PDF Dalton Transactions 40 33 8340 6 doi 10 1039 c1dt10840a OSTI 1051843 PMID 21766096 S2CID 33758070 Abergel R J Durbin P W Kullgren B Ebbe S N Xu J Chang P Y Bunin D I Blakely E A Bjornstad K A Rosen C J Shuh D K Raymond K N 2010 Biomimetic Actinide Chelators An Update on the Preclinical Development of the Orally Active Hydroxypyridonate Decorporation Agents 3 4 3 LI 1 2 HOPO and 5 LIO Me 3 2 HOPO Health Phys 99 3 401 407 doi 10 1097 HP 0b013e3181c21273 PMC 2921233 PMID 20699704 Panyala Nagender R Sturzbecher Hoehne Manuel Abergel Rebecca J 2014 Identification of process related trace level impurities in the actinide decorporation agent 3 4 3 LI 1 2 HOPO Nozzle skimmer fragmentation via ESI LC QTOFMS Journal of Pharmaceutical and Biomedical Analysis 100 157 166 doi 10 1016 j jpba 2014 08 004 PMC 4179986 PMID 25165012 An Dahlia D Kullgren Birgitta Jarvis Erin E Abergel Rebecca J 2017 From early prophylaxis to delayed treatment Establishing the plutonium decorporation activity window of hydroxypyridinonate chelating agents Chemico Biological Interactions 267 80 88 doi 10 1016 j cbi 2016 03 034 PMC 5045775 PMID 27038878 Abergel Rebecca J Ansoborlo Eric 2016 04 22 Curious curium Nature Chemistry 8 5 516 Bibcode 2016NatCh 8 516A doi 10 1038 nchem 2512 OSTI 1458477 PMID 27102687 S2CID 12473941 Deblonde Gauthier J P Sturzbecher Hoehne Manuel Abergel Rebecca J 2013 Solution Thermodynamic Stability of Complexes Formed with the Octadentate Hydroxypyridinonate Ligand 3 4 3 LI 1 2 HOPO A Critical Feature for Efficient Chelation of Lanthanide IV and Actinide IV Ions Inorganic Chemistry 52 15 8805 8811 doi 10 1021 ic4010246 PMC 3771511 PMID 23855806 Retrieved from https en wikipedia org w index php title Rebecca Abergel amp oldid 1161920172, wikipedia, wiki, book, books, library,

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