@article{ZalaStruszczykPeter2001,
  author    = {Zala, Eva and Struszczyk, Marcin Henryk and Peter, Martin G.},
  title     = {Effects of preparation methods for chitosan films on their properties},
  year      = {2001},
  language  = {en}
}
@article{BussVarumPeteretal.1996,
  author    = {Buss, U. and Varum, K. M. and Peter, Martin G. and Spindler-Barth, Margarethe},
  title     = {ELISA for quantitation of chitin, chitosan and related compounds},
  year      = {1996},
  language  = {en}
}
@article{AbegazPeter1995,
  author    = {Abegaz, Berhanu M. and Peter, Martin G.},
  title     = {Emodine and emodinanthrone rhamnoside acetates from fruits of rhamnus prinoides},
  issn      = {0031-9422},
  year      = {1995},
  language  = {en}
}
@article{TsukamotoHaebelValencaetal.2008,
  author    = {Tsukamoto, Junko and Haebel, Sophie and Valenca, Gustavo P. and Peter, Martin G. and FRanco, Telma T.},
  title     = {Enzymatic direct synthesis of acrylic acid esters of mono- and disaccharides},
  issn      = {0268-2575},
  year      = {2008},
  abstract  = {Background: There is an increased need to replace materials derived from fossil sources by renewables. Sugar- cane derived carbohydrates are very abundant in Brazil and are the cheapest sugars available in the market, with more than 400 million tons of sugarcane processed in the year 2007. The objective of this work was to study the prepn. of sugar acrylates from free sugars and free acrylic acid, thus avoiding the previous prepn. of protected sugar derivs., such as glycosides, or activated acrylates, such as vinyl acrylate. Results: Lipase catalyzed esterification of three mono- and two disaccharides with acrylic acid, in the presence or absence of mol. sieves was investigated. The reactions were monitored by high-performance liq. chromatog. (HPLC) and the products were analyzed by matrix-assisted laser desorption ionization-time of flight (MALDI-TOF) mass spectrometry. The main products are mono- and diacrylates, while higher esters are formed as minor products. The highest conversion to sugar acrylates was obsd. for the D-glucose and D- fructose, followed by D-xylose and D-maltose. Mol. sieves had no pronounced effect on the conversion. Conclusions: A feasible method is described to produce and to characterize sugar acrylates, including those contg. more than two acrylate groups. The process for prodn. of these higher esters could potentially be optimized further to produce mols. for crosslinking in acrylate polymn. and other applications. The direct enzymic esterification of free carbohydrates with acrylic acid is unprecedented. [on SciFinder (R)].},
  language  = {en}
}
@article{PereiraNascimentoMagalhaesetal.2014,
  author    = {Pereira, Fernanda S. and Nascimento, Heliara D. L. and Magalhaes, Alvicler and Peter, Martin G. and Bataglion, Giovana Anceski and Eberlin, Marcos N. and Gonzalez, Eduardo R. P.},
  title     = {ESI(+)-MS and GC-MS study of the hydrolysis of N-azobenzyl derivatives of chitosan},
  series = {Molecules},
  volume    = {19},
  journal   = {Molecules},
  number    = {11},
  publisher = {MDPI},
  address   = {Basel},
  issn      = {1420-3049},
  doi       = {10.3390/molecules191117604},
  pages     = {17604 -- 17618},
  year      = {2014},
  abstract  = {New N-p-chloro-, N-p-bromo-, and N-p-nitrophenylazobenzylchitosan derivatives, as well as the corresponding azophenyl and azophenyl-p-sulfonic acids, were synthesized by coupling N-benzylvchitosan with aryl diazonium salts. The synthesized molecules were analyzed by UV-Vis, FT-IR, H-1-NMR and N-15-NMR spectroscopy. The capacity of copper chelation by these materials was studied by AAS. Chitosan and the derivatives were subjected to hydrolysis and the products were analyzed by ESI(+)-MS and GC-MS, confirming the formation of N-benzyl chitosan. Furthermore, the MS results indicate that a nucleophilic aromatic substitution (SnAr) reaction occurs under hydrolysis conditions, yielding chloroaniline from N-p-bromo-, and N-p-nitrophenylazo-benzylchitosan as well as bromoaniline from N-p-chloro-, and N-p-nitrophenylazobenzyl-chitosan.},
  language  = {en}
}
@article{YenesewMidiwoHeydenreichetal.1998,
  author    = {Yenesew, Abiy and Midiwo, Jacob O. and Heydenreich, Matthias and Peter, Martin G.},
  title     = {Four isoflavanones from stem bark of erythrina sacleuxii},
  year      = {1998},
  language  = {en}
}
@article{OliveiraelGueddariMoerschbacheretal.2008,
  author    = {Oliveira, Enio N. and el Gueddari, Nour E. and Moerschbacher, Bruno M. and Peter, Martin G. and Franco, Telma T.},
  title     = {Growth of phytopathogenic fungi in the presence of partially acetylated chitooligosaccharides},
  issn      = {0301-486X},
  year      = {2008},
  abstract  = {Four phytopathogenic fungi were cultivated up to six days in media contg. chitooligosaccharide mixts. differing in av. DP and F A. The three different mixts. were named Q3 (which contained oligosaccharides of DP2-DP10, with DP2-DP7 as main components), Q2 (which contained oligosaccharides of DP2-DP12, with DP2-DP10 as main components) and Q1 (which derived from Q2 and contained oligomers of DP5-DP8 with hexamer and a heptamer as the main components). The novel aspect of this work is the description of the effect of mixts. of oligosaccharides with different and known compn. on fungal growth rates. The growth rate of Alternaria alternata and Rhizopus stolonifer was initially inhibited by Q3 and Q2 at higher concns. Q1 had a growth stimulating effect on these two fungi. Growth of Botrytis cinerea was inhibited by Q3 and Q2, while Q1 had no effect on the growth of this fungus. Growth of Penicillium expansum was only slightly inhibited by higher concns. of sample Q3, while Q2 and Q1 had no effect. The inhibition of growth rates or their resistance toward chitooligosaccharides correlated with the absence or presence of chitinolytic enzymes in the culture media, resp. [on SciFinder (R)]},
  language  = {en}
}
@article{HoustonShiomiAraietal.2002,
  author    = {Houston, Douglas R. and Shiomi, Kazuro and Arai, Noriko and Omura, Satoshi and Peter, Martin G. and Turberg, Andreas and Synstad, Bjoenar and Eijsink, Vincent G. H. and Van Aalten, Daan M. F.},
  title     = {High-resolution structures of a chitinase complexed with natural product cyclopentapeptide inhibitors : mimicry of carbohydrate substrate},
  year      = {2002},
  abstract  = {Over the past years, family 18 chitinases have been validated as potential targets for the design of drugs against human pathogens that contain or interact with chitin during their normal life cycles. Thus far, only one potent chitinase inhibitor has been described in detail, the pseudotrisaccharide allosamidin. Recently, however, two potent natural-product cyclopentapeptide chitinase inhibitors, argifin and argadin, were reported. Here, we describe high- resoln. crystal structures that reveal the details of the interactions of these cyclopeptides with a family 18 chitinase. The structures are examples of complexes of a carbohydrate-processing enzyme with high-affinity peptide-based inhibitors and show in detail how the peptide backbone and side chains mimic the interactions of the enzyme with chitooligosaccharides. Together with enzymol. characterization, the structures explain why argadin shows an order of magnitude stronger inhibition than allosamidin, whereas argifin shows weaker inhibition. The peptides bind to the chitinase in remarkably different ways, which may explain the differences in inhibition consts. The two complexes provide a basis for structure-based design of potent chitinase inhibitors, accessible by std. peptide chem.},
  language  = {en}
}
@misc{FerenzPeterBerg1983,
  author    = {Ferenz, Hans-J{\"u}rgen and Peter, Martin G. and Berg, Dieter},
  title     = {Inhibition of farnesoic acid methyltransferase by sinefungin},
  url       = {http://nbn-resolving.de/urn:nbn:de:kobv:517-opus-17016},
  year      = {1983},
  abstract  = {Sinefungin inhibited the S-adenosylmethionine-dependent farnesoic acid methyltransferase in a cell-free system containing a homogenate of corpora allata from female locusts, Locusta migratoria. The enzyme catalyzed the penultimate step of juvenile hormone biosynthesis in the insects. Culturing corpora allata in the presence of sinefungin greatly suppressed juvenile hormone production. The following in vivo effects were visible after injection of the inhibitor: increase in mortality and reduction of total haemolymph protein liter and ovary fresh weight, as well as length of terminal oocytes. Attempts to reverse these effects by topical application of the juvenile hormone analog ZR-515 (methoprene) were only partly successful. Therefore, the in vivo effects may be due to a general inhibition of methyltransferase enzymes in the insect. Sinefungin appeared to be of potential interest as the first representative of a new class of insect growth regulators.},
  language  = {en}
}
@article{KaatzStrefferWollenbergeretal.1999,
  author    = {Kaatz, Helvi and Streffer, Katrin and Wollenberger, Ursula and Peter, Martin G.},
  title     = {Inhibition of mushroom tyrosinase by kojic acid octanoates},
  year      = {1999},
  language  = {en}
}
@article{VaajeKolstadVasellaPeteretal.2004,
  author    = {Vaaje-Kolstad, G. and Vasella, A. and Peter, Martin G. and Netter, C. and Houston, Douglas R. and Westereng, B. and Synstad, Bjoenar and Eijsink, Vincent G. H. and van Aalten, Daan M. F.},
  title     = {Interactions of a family 18 chitinase with the designed inhibitor HM508 and its degradation product, chitobiono- delta-lactone},
  issn      = {0021-9258},
  year      = {2004},
  abstract  = {We describe enzymological and structural analyses of the interaction between the family 18 chitinase ChiB from Serratia marcescens and the designed inhibitor N,N'-diacetylchitobionoxime-N-phenylcarbamate (HM508). HM508 acts as a competitive inhibitor of this enzyme with a K-i in the 50 muM range. Active site mutants of ChiB show K-i values ranging from 1 to 200 muM, providing insight into some of the interactions that determine inhibitor affinity. Interestingly, the wild type enzyme slowly degrades HM508, but the inhibitor is essentially stable in the presence of the moderately active D142N mutant of ChiB. The crystal structure of the D142N-HM508 complex revealed that the two sugar moieties bind to the -2 and -1 subsites, whereas the phenyl group interacts with aromatic side chains that line the +1 and +2 subsites. Enzymatic degradation of HM508, as well as a Trp-->Ala mutation in the +2 subsite of ChiB, led to reduced affinity for the inhibitor, showing that interactions between the phenyl group and the enzyme contribute to binding. Interestingly, a complex of enzymatically degraded HM508 with the wild type enzyme showed a chitobiono-delta- lactone bound in the -2 and -1 subsites, despite the fact that the equilibrium between the lactone and the hydroxy acid forms in solution lies far toward the latter. This shows that the active site preferentially binds the E-4 conformation of the -1 sugar, which resembles the proposed transition state of the reaction},
  language  = {en}
}
@article{BringmannMutanyattaComarMaksimenkaetal.2008,
  author    = {Bringmann, Gerhard and Mutanyatta-Comar, Joan and Maksimenka, Katja and Wanjohi, John M. and Heydenreich, Matthias and Brun, Reto and M{\"u}ller, Werner E. G. and Peter, Martin G. and Midiwo, Jacob O. and Yenesew, Abiy},
  title     = {Joziknipholones A and B : the first dimeric phenylanthraquinones, from the roots of Bulbine frutescens},
  issn      = {0947-6539},
  year      = {2008},
  abstract  = {From the roots of the African plant Bulbine frutescens (Asphodelaceae), two unprecedented novel dimeric phenylanthraquinones, named joziknipholones A and B, possessing axial and centrochirality, were isolated, together with six known compounds. Structural elucidation of the new metabolites was achieved by spectroscopic and chiroptical methods, by reductive cleavage of the central bond between the monomeric phenylanthraquinone and -anthrone portions with sodium dithionite, and by quantum chemical CD calculations. Based on the recently revised absolute axial configuration of the parent phenylanthraquinones, knipholone and knipholone anthrone, the new dimers were attributed to possess the P- configuration (i.e., with the acetyl portions below the anthraquinone plane) at both axes in the case of joziknipholone A, whereas in joziknipholone B, the knipholone part was found to be M-configured. Joziknipholones A and B are active against the chloroquine resistant strain K1 of the malaria pathogen, Plasmodium falciparum, and show moderate activity against murine leukemic lymphoma L5178y cells.},
  language  = {en}
}
@article{LetzelSynstadEijsinketal.1999,
  author    = {Letzel, Matthias C. and Synstad, Bjoenar and Eijsink, Vincent G. H. and Peter-Katalinic, Jasna and Peter, Martin G.},
  title     = {Libraries of chito-oligosaccharides of mixed acetylation patterns and their interactions with chitinases},
  isbn      = {3-9806494-5-8},
  year      = {1999},
  language  = {en}
}
@article{IssareeVijayakrishnanAbdelnuretal.2009,
  author    = {Issaree, Arisara and Vijayakrishnan, Balakumar and Abdelnur, Patricia V. and Corilo, Yuri E. and Riccio, Maria F. and Sanvido, Gustavo B. and Eberlin, Marcos N. and Peter, Martin G.},
  title     = {Mass spectrometry of aminoglucan oligosaccharides using electrospray ionization MS/MS and MS/MS/MS},
  year      = {2009},
  language  = {en}
}
@article{LetzelPeterKatalinicPeter2001,
  author    = {Letzel, Matthias C. and Peter-Katalinic, Jasna and Peter, Martin G.},
  title     = {Mass spectrometry of chitin and chitosan oligosaccharides},
  year      = {2001},
  language  = {en}
}
@article{HaebelPeterKatalinicPeter1997,
  author    = {Haebel, Sophie and Peter-Katalinic, Jasna and Peter, Martin G.},
  title     = {Mass spectrometry of chitooligosaccharides},
  isbn      = {88-86889- 01-1},
  year      = {1997},
  language  = {en}
}
@article{StruszczykLothPeter1999,
  author    = {Struszczyk, Marcin Henryk and Loth, Fritz and Peter, Martin G.},
  title     = {Method of microcrystalline chitosan-protein films preparation},
  year      = {1999},
  language  = {en}
}
@article{NorledgeLambeirAbagyanetal.2001,
  author    = {Norledge, Brian V. and Lambeir, Anne M. and Abagyan, Ruben and Rottmann, Antje and Fernendez, Anna M. and Filimonov, Vladimir V. and Peter, Martin G. and Wierenga, Rik K.},
  title     = {Modeling, mutagenesis, and structural studies on the fully conserved phoshate-binding loop (Loop 8) of triosephosphate isomerase : toward a new substrate specificity},
  issn      = {0887-2585},
  year      = {2001},
  language  = {en}
}
@article{VijayakrishnanIssareeCoriloetal.2011,
  author    = {Vijayakrishnan, Balakumar and Issaree, Arisara and Corilo, Yuri E. and Ferreira, Christina Ramires and Eberlin, Marcos N. and Peter, Martin G.},
  title     = {MSn of the six isomers of (GlcN)(2)(GlcNAc)(2) aminoglucan tetrasaccharides (diacetylchitotetraoses) rules of fragmentation for the sodiated molecules and application to sequence analysis of hetero-chitooligosaccharides},
  series = {Carbohydrate polymers : an international journal devoted to scientific and technological aspects of industrially important polysaccharides},
  volume    = {84},
  journal   = {Carbohydrate polymers : an international journal devoted to scientific and technological aspects of industrially important polysaccharides},
  number    = {2},
  publisher = {Elsevier},
  address   = {Oxford},
  issn      = {0144-8617},
  doi       = {10.1016/j.carbpol.2010.04.041},
  pages     = {713 -- 726},
  year      = {2011},
  abstract  = {The six possible isomers of di-N-acetylchitotetraoses [AADD, ADDA, ADAD, DADA, DAAD, and DDAA, where D stands for 2-amino-2-deoxy-3-D-glucose (GlcN) and A for 2-acetamido-2-deoxy-beta-D-glucose (GlcNAc)] were analyzed by ESI(+)-MSn. Collision induced dissociation via MSn experiments were performed for the sodiated molecules of m/z 769 [M+Na](+) for each isomer, and fragments were generated mainly by glycosidic bond and cross-ring cleavages. Rules of fragmentation were then established. A reducing end D residue yields the (O.2)A(4) cross-ring [M-59+Na](+) fragment of m/z 710 as the most abundant, whereas isomers containing a reducing end A prefer to lose water to form the [M-18+Na](+) ion of m/z 751, as well as abundant (O.2)A(4) cross-ring [M-101+Na](+) fragments of m/z 668 and B-3 [M-221+Na](+) ions of m/z 548. MS3 of C- and Y-type ions shows analogous fragmentation behaviour that allows identification of the reducing end next-neighbour residue. Due to gas-phase anchimeric assistance, B-type cleavage between the glycosidic oxygen and the anomeric carbon atom is favoured when the glycon is an A residue. Relative ion abundances are generally in the order B >> C > Y, but may vary depending on the next neighbour towards the non-reducing end. These fragmentation rules were used for partial sequence analysis of hetero-chitooligosaccharides of the composition D(2)A(3), D(3)A(3), D(2)A(4), D(4)A(3), and D(3)A(4).},
  language  = {en}
}
@article{Peter2001,
  author    = {Peter, Martin G.},
  title     = {Nat{\"u}rliche Klebstoffe : von Muscheln, Seepocken, Spinnen und anderem Klebe-Getier},
  isbn      = {3-519-16195-8},
  year      = {2001},
  language  = {de}
}