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1

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Inhibition by tetanus and botulinum A toxin of the release of [3H]noradrenaline and [3H]GABA from rat brain homogenate (1988)

Habermann, E.

Springer

Cellular and molecular life sciences 44 (1988), S. 224-226

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ISSN: 1420-9071

Keywords: Tetanus toxin ; botulinum toxin ; noradrenaline ; GABA ; brain

Source: Springer Online Journal Archives 1860-2000

Topics: Biology , Medicine

Notes: Summary Rat brain homogenate was preloaded with [3H]noradrenaline or [3H]GABA and stimulated with high K+. Tetanus toxin and botulinum A neurotoxin partially prevent the evoked [3H]noradrenaline release in the same range of toxin concentrations starting below 10−10M. In contrast, release of γ-amino butyric acid (GABA) is much more sensitive to tetanus than to botulinum A toxin.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01941714

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Advances in tetanus research (1974)

Habermann, E. ; Wellhöner, H. H.

Springer

Journal of molecular medicine 52 (1974), S. 255-265

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ISSN: 1432-1440

Keywords: Tetanus toxin ; Antitoxin ; 125Iodine ; Spinal cord ; Nerves ; Tetanustoxin ; Antitoxin ; 125Jod ; Rückenmark ; Nerven

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Description / Table of Contents: Zusammenfassung Unsere Kenntnis der Pathogenese des Wundstarrkrampfes hat sich durch Anwendung neuer biochemischer und neurophysiologischer Techniken innerhalb der letzten Jahre erheblich erweitert. Radioaktiv markiertes Tetanustoxin wurde innerhalb verschiedener Nerven bis zu den Vorderhörnern des Rückenmarks verfolgt; dort wurde das Toxin z.T. noch auf cellulärer Ebene nachgewiesen. Die Verteilung des Toxins ist zeitabhängig und wird durch Antitoxin beeinflußt. Je weiter der Zeitpunkt der Vergiftung zurückliegt, desto geringer ist der Effekt des Antitoxins auf die Symptomatologie und die spinale Anreicherung des Toxins. Die neurale Wanderung des Toxins wird durch Erregung des toxinhaltigen Nerven gefördert. Neben den motorischen Anteilen sind auch rein sensibel-sensorische und vegetative Nerven zur Weiterleitung des Toxins imstande. Der generalisierte Tetanus kann als eine Sonderform des lokalen Tetanus betrachtet werden. Während bisher das klassische α-motorische System des Rückenmarks im Vordergrund der Untersuchungen stand, weisen neuere Arbeiten auf eine gleichzeitige, vielleicht sogar vorwiegende Enthemmung des γ-motorischen Systems hin. Außerdem werden vegetative Spinalreflexe enthemmt, was auch bei der Therapie bedacht werden sollte. Die Hemmwirkung des Tetanustoxins auf periphere Synapsen weist auf große Ähnlichkeiten mit Botulinumtoxin hin, obwohl die Symptome am vergifteten Tier so verschieden sind. Künftige Untersuchungen werden sich voraussichtlich mit der Wirkungsweise des Toxins auf molekularer und cellulärer Ebene befassen.

Notes: Summary Due to the use of advanced biochemical and neurophysiological techniques, our knowledge of the pathogenesis of tetanus has considerably improved during the past years. Radio-labelled tetanus toxin has been traced within different nerves up to the anterior horn of the spinal cord where its localization down to the cellular level has been achieved. The distribution of labelled toxin depends on time and is influenced by antitoxin. The longer the duration of poisoning, the smaller the effect of antitoxin on the spinal enrichment of toxin and on the onset of toxic symptoms. The neural ascent of toxin into a spinal cord segment is enhanced by stimulation of the segmental nerves. Not only the motor nerves, but also sensory and vegetative nerves are able to serve as guide-rails for the toxin. The generalized tetanus has been understood as a special kind of local tetanus. For a long time, disinhibition of the alpha motor system was considered to be the characteristic action of tetanus toxin, but recent evidence is in favour of an additional disinhibition of the gamma motor system (perhaps even preceding the alpha disinhibition) and also of the sympathetic spinal reflexes. This finding should have therapeutic implications. The detection of inhibitory effects of tetanus toxin on peripheral cholinergic synapses points again to the close similarity between tetanus toxin and botulinum A toxin. The trends of future research will presumably lead to the elementary processes at the molecular and cellular level which are the basis of the clinical picture of tetanus.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01468455

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Production of biologically active light chain of tetanus toxin in Escherichia coli - Evidence for the importance of the C-terminal 16 amino acids for full biological activity

Fairweather, N.F. ; Sanders, D. ; Slater, D. ; [et al.]

Amsterdam : Elsevier

FEBS Letters 323 (1993), S. 218-222

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ISSN: 0014-5793

Keywords: E. coli, Chromaffin cell ; Exocytosis ; Recombinant protein ; Site directed mutagenesis ; Tetanus toxin

Source: Elsevier Journal Backfiles on ScienceDirect 1907 - 2002

Topics: Biology , Chemistry and Pharmacology , Physics

Type of Medium: Electronic Resource

URL: http://linkinghub.elsevier.com/retrieve/pii/0014-5793(93)81343-X

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The tetanus toxin light chain inhibits exocytosis

Ahnert-Hilger, G. ; Weller, U. ; Dauzenroth, M.-E. ; [et al.]

Amsterdam : Elsevier

FEBS Letters 242 (1989), S. 245-248

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ISSN: 0014-5793

Keywords: (Chromaffin cell) ; Exocytosis ; Light chain ; Streptolysin O ; Tetanus toxin

Source: Elsevier Journal Backfiles on ScienceDirect 1907 - 2002

Topics: Biology , Chemistry and Pharmacology , Physics

Type of Medium: Electronic Resource

URL: http://linkinghub.elsevier.com/retrieve/pii/0014-5793(89)80478-8

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Light chain of tetanus toxin intracellularly inhibits acetylcholine release at neuro-neuronal synapses, and its internalization is mediated by heavy chain

Mochida, S. ; Poulain, B. ; Weller, U. ; [et al.]

Amsterdam : Elsevier

FEBS Letters 253 (1989), S. 47-51

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ISSN: 0014-5793

Keywords: (Aplysia) ; Central synapse ; Heavy chain ; Light chain ; Tetanus toxin ; Transmitter release

Source: Elsevier Journal Backfiles on ScienceDirect 1907 - 2002

Topics: Biology , Chemistry and Pharmacology , Physics

Type of Medium: Electronic Resource

URL: http://linkinghub.elsevier.com/retrieve/pii/0014-5793(89)80926-3

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Isolierung und Struktur peptischer kininliefernder Peptide aus Rinderserum (1969)

Jahrreiss, R. ; Habermann, E.

Springer

Naunyn-Schmiedeberg's archives of pharmacology 264 (1969), S. 172-186

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ISSN: 1432-1912

Keywords: Bovine Serum ; Kininogen ; Peptides ; Enzymes ; Structure Evaluation ; Rinderserum ; Kininogen ; Peptide ; Enzyme ; Struktur-aufklärung

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Description / Table of Contents: Zusammenfassung 1. Rinderserum ergab beim Umsatz mit Pepsin niedermolekulare, kininliefernde Spaltstücke. Das durch Fällung, Verteilung, Gelfiltration und Jonenaustausch-Chromatographie vorgereinigte Hydrolysat ließ sich durch Papierchromatographie in 2 Fraktionen trennen, auf die sich die kininliefernde Gruppierung im Verhältnis 5∶1 verteilte. 2. Beide kininliefernde Fraktionen waren resistent gegen Carboxypeptidase B, was gegen eine C-terminale Position der Kininsequenz spricht. Sie waren aktivierbar durch Trypsin, Pankreaskallikrein und auch Carboxypeptidase A. Trypsin in höherer Konzentration entwickelte aus der Hauptfraktion (L) Bradykinin, während mit Pankreaskallikrein, Carboxypeptidase A und kleinen Trypsinmengen Met-Lys-Bradykinin entstand. Die „direkte“ Aktivität der Fraktionen am Meerschweinchenileum lag bei maximal 1–2% der „indirekten“. 3. Aus der chromatographisch langsameren Hauptfraktion (L) wurde hoch-spannungselektrophoretisch ein einheitliches Minimalsubstrat für Kininogenasen isoliert. In seiner Aminosäurenanalyse entsprach es dem aus gereinigtem Rinderserum-Kininogen isolierten Hauptpeptid PKFL; auch beim Edman-Abbau ergaben sich keine Unterschiede. 4. Die früher für gereinigtes Kininogen beschriebenen Sequenzen sind also auch für Gesamtserum repräsentativ. Hinweise auf andersartige Peptide, insbesondere auf solche mit der Kininsequenz in C-terminaler Position, ergaben sich nicht.

Notes: Summary 1. Peptic treatment of bovine serum produced kinin yielding substances of low molecular weight. The hydrolyzate was purified by precipitation, partition, gel filtration and ion exchange chromatography. Subsequent paper chromatography revealed two fractions with a 5∶1 distribution of the kinin-yielding property. 2. Both kinin-yielding fractions were resistant to carboxypeptidase B, a finding which argues against a C-terminal position of the kinin sequence. They could be activated by trypsin, pancreatic kallikrein, and carboxypeptidase A. Higher concentrations of trypsin released bradykinin from the main fraction (L), whereas pancreatic kallikrein, carboxypeptidase A and low amounts of trypsin produced met-lysbradykinin. The “direct” activity of the fractions as measured on the guinea pig ileum was no more than 1–2% of the “indirect” activity. 3. A homogeneous minimal substrate was isolated from the chromatographically slower fraction L by high voltage electrophoresis. With respect to amino acid analysis and Edman degradation, it could not be distinguished from the peptide PKFL isolated from purified bovine kininogen. 4. Therefore, the sequences described previously in purified kininogen are also representative for whole serum. Evidence for different peptides, especially with the kinin sequence in C-terminal position, was not found.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00997326

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Inhibition of synaptosomal choline uptake by tetanus and botulinum a toxin (1981)

Habermann, E. ; Bigalke, H. ; Heller, Irmtraud

Springer

Naunyn-Schmiedeberg's archives of pharmacology 316 (1981), S. 135-142

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ISSN: 1432-1912

Keywords: Tetanus toxin ; Botulinum A toxin ; Choline ; Gangliosides ; Fixation

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Tetanus toxin and, to a lesser degree, botulinum A toxin inhibit partially and noncompetitively the uptake of [3H]choline into a crude synaptosomal fraction from rat brain cortex. Botulinum toxin acts by its neurotoxin content. The effect is not due to nonspecific synaptosomal damage by the toxins as shown by the lactate dehydrogenase occlusion test, by the absence of swelling and by the preservation of choline stores. The ratio between [3H]acetylcholine and [3H]choline was decreased by both toxins. Inhibition by either toxin depends strongly on the temperature and duration of incubation, and is preceded by an initial latency period. The effect of tetanus toxin, once manifest, is largely resistant against antitoxin. It is not significantly diminished by pretreatment of the synaptosomes with V. cholerae neuraminidase. Fixation of 125I-tetanus toxin proceeds fast, is largely independent of temperature and is diminished by pretreatment of the synaptosomes with neuraminidase. Thus only some of the fixation sites, and not the long-chain gangliosides, are required for the effects of tetanus toxin. A slow, temperature-sensitive process links the fixation with the action. In contrast to rat synaptosomes the chicken preparation is more sensitive to botulinum A than to tetanus toxin, which reflects the differences in sensitivity between live birds and rodents. Our data underline the similarities between the effects of tetanus and those of botulinum A toxin. Their dependence on time and temperature, the time dependence of efficacy of antitoxin, and the concordance in species specificity indicate that the in vitro system mirros some crucial features of poisoning of isolated organs and live animals.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00505307

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Mastzelldegranulierendes Peptid (MCD-Peptid) aus Bienengift: Isolierung, biochemische und pharmakologische Eigenschaften (1968)

Breithaupt, H. ; Habermann, E.

Springer

Naunyn-Schmiedeberg's archives of pharmacology 261 (1968), S. 252-270

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ISSN: 1432-1912

Keywords: Peptides ; Bee Venom ; Mast Cells ; Histamine ; Vascular Permeability ; Peptide ; Bienengift ; Mastzellen ; Histamin ; Gefäßpermeabilität

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Description / Table of Contents: Zusammenfassung Bienengift enthält neben dem universell zellschädigenden Melittin und der über Lysolecithinbildung wirksamen Phospholipase A ein drittes mastzelldegranulierendes (MCD-)Peptid. Seine Isolierung gelingt durch Kombination von Gelfiltration an Sephadex G 50 mit Ionenaustauschchromatographie an Carboxymethylcellulose und an Amberlite IRC-50. MCD-Peptid ist stark basisch (Isoelektrischer Punkt um pH 12). Sein minimales Molekulargewicht errechnet sich aus der Aminosäurenanalyse zu 2593. Das Peptid besteht aus 22 Aminosäuren, darunter 4 Halbcystinen. Es liegt in zwei verschiedenen Ladungszuständen vor, die sich bei Papierchromatographie, Papierelektrophorese und Aminosäurenanalyse einheitlich verhalten. MCD-Peptid ist an isolierten Rattenmastzellen (Histaminfreisetzung) und am Mesenterialhäutchen der Ratte (Mastzelldegranulation) etwa wirkungsgleich mit dem synthetischen Histaminliberator Compound 48/80. Melittin wirkt ca. 100- bzw. 10 mal schwächer und zeichnet sich überdies durch eine sehr flache Dosis-Wirkungsbeziehung bei der Histaminfreisetzung aus. Der Rattenblutdruck wird durch MCD-Peptid und Compound 48/80 in quantitativ und qualitativ vergleichbarer Weise gesenkt. Zwischen beiden Substanzen besteht kreuzweise Tachyphylaxie. Die Permeabilität der Hautgefäße der Ratte für zirkulierendes Evans-Blau steigt bei intracutaner Applikation von MCD-Peptid und Compound 48/80. Beide Substanzen sind hier stärker wirksam als Melittin. Die Hautgefäße des Kaninchens sprechen jedoch auf MCD-Peptid schwächer an als auf Melittin und Compound 48/80. Die Ratte reagiert auf i.v. Injektion von 0,5–10 mg/kg MCD-Peptid mit massiver Hyperämie der Acren. Eine kurzdauernde Spastik der Extremitäten weist auf einen zusätzlichen Angriff am motorischen System hin.

Notes: Summary Bee venom contains three agents which can produce mast cell degranulation. Melittin is a universally acting surfactant; phospholipase A releases the mastocytolytic lysolecithin. A third mast cell degranulating (MCD) peptide has been isolated by gel filtration on Sephadex G 50, followed by chromatography on carboxymethylcellulose, and, finally, on Amberlite IRC-50. MCD-peptide is strongly basic (isoelectric point near pH 12). From the amino acid analysis, a minimum molecular weight of 2593 has been calculated. MCD-peptide consists of 22 amino acids, among them 4 halfcystine residues. It can be obtained in two fractions differing by charge, which appear homogeneous, however, on paper chromatography, paper electrophoresis, and amino acid analysis. When tested on isolated mast cells or on mesentery tissue of rats, MCD-peptide is equiactive with compound 48/80. On the other hand, melittin is 100 times less potent than compound 48/80 on the former tissue and 10 times less potent on the latter; moreover, the dose-response-relation of histamine release is flatter with melittin. MCD-peptide and compound 48/80 depress the blood pressure of rats in a quantitatively and qualitatively similar manner. Crossed tachyphylaxis has been demonstrated. Both substances increase the capillary permeability of rat skin upon intracutaneous injection. Melittin is less active on rat skin vessels. The skin capillaries of rabbits are, however, more sensitive to melittin and compound 48/80 than to MCD-peptide. MCD-peptide (0.5–10 mg/kg i.v.) produces in rats an extreme cyanosis of the acra. A short lasting spasm of the extremities points to an additional effect on the motor system of rats.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00536989

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Comparative studies of native and synthetic melittins (1971)

Habermann, E. ; Zeuner, G.

Springer

Naunyn-Schmiedeberg's archives of pharmacology 270 (1971), S. 1-9

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ISSN: 1432-1912

Keywords: Melittin ; Peptides ; Venoms ; Hemolysis

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The hexacosapeptide melittin I, which is the main toxin of bee venom, has been synthesized by Lübke and Schröder. In addition, the following derivatives have been prepared which are probably also present in bee venom: melittin II (which differs by one serine), and N1-formylated melittin I and II. In pharmacological tests, the four synthetic peptides were qualitatively indistinguishable from natural melittin as prepared from bee venom. Theyhemolyzed rabbit erythrocytes with a flat dose-response curve. Melittin I exerted 92% of the activity of the natural substance, the three other peptides 90, 61 and 52% respectively.-Theirsurface activity was between 86 and 96% of that of the natural material.-In contrast to our previous reports, no differences were found in onset, degree and duration of the shortlastinghypotensive action in rabbits.-Toxicity (LD 50, mice) was about 4 mg/kg for natural melittin and for the synthetic melittins I and II. The toxicity of formylated melittins was not very different.-The five compounds caused a slow and prolongedcontraction of the guinea-pig ileum which led to tachyphylaxis. Peptide mapping confirmed the identity between the main compound of natural melittin and synthetic melittin I. The peptide pattern of synthetic melittin II is different and is further modified by the presence of the N-formyl group. Our findings leave no doubt as to the identity between the bulk of natural melittin and melittin I. They corroborate the presence in natural melittin of small amounts of N1-formylated melittin I. The pharmacological similarities to synthetic melittin II and N1-formylated melittin II (which have not yet been identified in the venom) argue for a broader structural basis of the melittins as a group.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00997294

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Blockade by tetanus and botulinum A toxin of postganglionic cholinergic nerve endings in the myenteric plexus (1980)

Bigalke, H. ; Habermann, E.

Springer

Naunyn-Schmiedeberg's archives of pharmacology 312 (1980), S. 255-263

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ISSN: 1432-1912

Keywords: Acetylcholine ; Tetanus toxin ; Botulinum toxin ; Myenteric plexus ; Transmitter release

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The effects of tetanus and botulinum A toxin were studied on the electrically stimulated myenteric plexus-ileum strip of the guinea pig. The concentrations used were in the range of 104–106 mouse LD50/ml. 1. Tetanus and botulinu, A toxin slowly decrease the amplitude of the contractile response to field stimulation in a dose-dependent manner without influencing the sensitivity to acetylcholine of the smooth muscle. 2. Development of paralysis is preceded by a latent period. Washing and antitoxin slow the paralytic process only when applied during the latent period. 3. The time course of development of paralysis depends on the activity of the strip. It can be slowed by rest, high [Mg2+], or low [Ca2+], and accelerated by raising the stimulation frequency. 4. Substances like 4-aminopyridine, sea anemone toxin II and scorpion toxin which prolong the membrane depolarization restore temporarily the contraction of partially paralysed muscle strips. 5. Poisoned preparations do not differ from controls in their total acetylcholine contents, whereas formation as well as release of [3H]-acetylcholine are decreased by either toxin. It is concluded that a) tetanus toxin and botulinum A toxin are qualitatively indistinguishable with respect to their actions on the postganglionic cholinergic neurons in the ileum, botulinum A toxin being 5 times more potent than tetanus toxin, b) the effects of the toxins at postganglionic cholinergic neurons in the ileum and at motor nerve endings are qualitatively similar, botulinum A toxin being about 500 times more potent than tetanus toxin at the latter preparation (see Habermann et al., 1980b, c) both toxins influence the turnover of acetylcholine but not its tissue concentration.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00499155

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