This document provides an overview of bacterial toxins, classifying them into two main categories: exotoxins that act on specific host sites, and toxins that act intracellularly or on the cell surface. It describes various toxin classes, including their mechanisms of action, examples of toxins that fall into each class, and the consequences of their activities. The classes discussed include toxins that act on the immune system, surface molecules, through pore formation, using the RTX mechanism, by perturbing membranes, targeting insects, and those acting intracellularly on protein synthesis, signal transduction pathways, and other targets. Specific toxins are given for each class along with their producing organisms and molecular activities.

1. Bacterial
Toxins
Classification
Dr.Faghri
Meisam.Roozbahani

2. Introduction

Toxins were the first bacterial virulence factors to
be identified and were also the first link between
bacteria and cell biology.

3. Introduction

Cellular microbiology was, in fact, naturally born
a long time ago with the study of toxins, and only
recently, thanks to the sophisticated new
technologies, has it expanded to include the study
of many other aspects of the interactions
between bacteria and host cells.

4. Two Main Categories of Toxins

7. Specific Host Site Exotoxins

Neurotoxins

Enterotoxins

Cytotoxins

Nephrotoxin

Hepatotoxin

Cardiotoxin

8. Classification by Entrance Mechanism

9. Injected into
eukaryotic cells
Protein synthesis
Mediators of apoptosis
Surface molecules
Signal transduction
Inositol phosphate
metabolism
Cell membrane
Class
Acting on
intracellular
targets
Immune system
(Superantigens)
Target
Acting on the
cell surface
Cytoskeleton structure
Cytoskeleton
Large pore- forming toxins
Intracellular trafficking
Signal transduction
Small pore- forming toxins
RTX toxins
Membrane-perturbing
toxins
Other pore- forming
toxins
Insecticidal toxins
Unknown
mechanism of
action

10. Toxins acting on the cell surface:
Immune system (Superantigens)

Superantigens are bacterial
and viral proteins that share
the ability to activate a large
fraction of T-lymphocytes.

11. Toxins acting on the cell surface: Immune system (Superantigens)
Toxin
Organism
Activity
Consequence
Binding to MHC class II
molecules and to Vβ or Vγ
of T cell receptor
T cell activation and
cytokines secretion
MAM
Mycoplasma
arthritidis
Binding to MHC class II
molecules and to Vβ or Vγ
of T cell receptor
Chronic inflammation
YPMa
Yersinia
pseudotuberculosis
Binding to MHC class II
molecules and to Vβ or Vγ
of T cell receptor
Chronic Inflammation
S. pyogenes
Cysteine protease
Alteration in
Immunoglobulin binding
properties
S. aureus
Trypsin-like serine
proteases
T-cell proliferation,
intraepidermal layer
separation
SEA-SEI, TSST-1, SPEA,
Staphylococcus
SPEC, SPEL, SPEM, SSA, and aureus and Streptococcus
SMEZ
pyogenes
SPEB
ETA, ETB, and ETD

12. Agr Regulatory System

13. Toxins acting on the cell surface:
Surface molecules

BFT enterotoxin: The pathogenicity of ETBF is
ascribed to a heat-labile ∼20-kDa toxin (B.
fragilis toxin [BFT], also called fragilysin).

This toxin binds to a specific intestinal epithelial
cell receptor and stimulates cell proliferation.

14. BFT enterotoxin

15. Toxins acting on the cell surface: Surface molecules
Toxin
Organism
Activity
Consequence
BFT enterotoxin
Bacteroides fragilis
Metalloprotease, cleavage
of E-cadherin
Alteration of epithelial
permeability
AhyB
Aeromonas
hydrophyla
Elastase,
metalloprotease
Hydrolization of casein and
elastine
Aminopeptidase
Pseudomonas
aeruginosa
Elastase,
metalloprotease
Corneal infection,
inflammation and
ulceration
ColH
Clostridium
histolyticum
Collagenase,
metalloprotease
Collagenolytic activity
Nhe
Bacillus cereus
Metalloprotease and
collagenase
Collagenolytic activity

16. Toxins acting on the cell surface:
Pore-Forming

Protein toxins forming pores in biological membranes
occur frequently in Gram-positive and Gram-negative
bacteria.

Pore-forming toxins, also known as "lytic factors".

Some of them are also called "hemolysins“.

17. Toxins acting on the cell surface:
Large Pore-Forming Toxins

Generally secreted by diverse species of Grampositive bacteria.

Binding selectively to cholesterol on the
eukaryotic cell membrane.

18. Toxins acting on the cell surface: Large pore forming toxins
Toxin
Organism
Activity
Consequence
PFO
C. perfringens
Thiol-activated cytolysin,
cholesterol Binding
Gas gangrene
SLO
S. pyogenes
Thiol-activated cytolysin,
cholesterol Binding
Transfer of other toxins,
cell death
Induction of Lymphocyte
apoptosis
Membrane damage
Induction of Lymphocyte
Apoptosis
Complement activation,
cytokine production,
apoptosis
LLO
Pneumolysin
Listeria monocytogenes
S. pneumoniae

19. Toxins acting on the cell surface:
Small pore forming toxins

Creating very small pores 1-1.5 nm diameter.

Selective permeabilization to solutes with a molecular
mass less than 2 kDa.

20. Toxins acting on the cell surface: Small pore forming toxins
Toxin
Organism
Activity
Consequence
Alveolysin
B. alveis
Induction of lymphocyte Apoptosis
Complement activation, cytokine
production, apoptosis
ALO
B. anthracis
Induction of lymphocyte apoptosis
Complement activation, cytokine
production, Apoptosis
α-Toxin
S. aureus
Binding of erythrocytes
Release of cytokines, cell lysis, apoptosis
PVL leukocidin
(LukS-LukF)
S. aureus
Cell membrane permeabilization
Necrotic enteritis, rapid shock-like
syndrome
γ-Hemolysins
(HlgA- HlgB and
HlgC- HlgB)
S. aureus
Cell membrane permeabilization
Necrotic enteritis, rapid shock-like
syndrome
β-Toxin
C. perfringens
Cell membrane permeabilization
Necrotic enteritis, neurologic effects

21. Toxins acting on the cell surface:
RTX toxins

The RTX toxin family is a group of cytotoxins produced by
Gram-negative bacteria.

There are over 1000 known members with a variety of
functions.

22. Toxins acting on the cell surface:
RTX toxins

The RTX family is defined by two common features:
characteristic repeats in the toxin protein sequences, and
extracellular secretion by the type I secretion system
(T1SS).

The name RTX (repeats in toxin) refers to the glycine and
aspartate-rich repeats located at the C-terminus of the
toxin proteins.

23. Genomic Structure

The toxin is encoded by four genes, one of which, hlyA,
encodes the 110-kDa hemolysin. The other genes are
required for its posttranslational modification (hlyC) and
secretion (hlyB and hlyD).

24. Toxins acting on the cell surface: RTX toxins
Toxin
Organism
Activity
Consequence
Hemolysin II
B. cereus
Cell membrane permeabilization
Hemolytic activity
CytK
B. cereus
Cell membrane Permeabilization
Necrotic enteritis
HlyA
E. coli
Calcium-dependent formation of transmembrane Pores
Cell permeabilization and lysis

25. Toxins acting on the cell surface:
Membrane perturbing toxins

Soap like structure.

The toxin binds nonspecifically parallel to the surface of
any membrane without forming transmembrane channels.

Cells first become permeable to small solutes and
eventually swell and lyse, releasing cell intracellular
content.

26. Toxins acting on the cell surface: Membrane perturbing toxins
Toxin
Organism
Activity
Consequence
ApxI, ApxII, and ApxIII A.pleuropneumoniae
Calcium-dependent formation of
transmembrane Pores
Lysis of erythrocytes and
other nucleated Cells
LtxA
A.actinomycetemcomitans
Calcium-dependent formation of
transmembrane Pores
Apoptosis
LtxA
P.Haemolytica
Calcium-dependent formation of
transmembrane Pores
Activity specific versus
ruminant leukocytes

27. Toxins acting on the cell surface:
Other pore forming toxins

Like other functionally related toxins, aerolysin changes
its topology in a multi-step process from a completely
water-soluble form to a membrane-soluble heptameric
transmembrane channel that destroys sensitive cells by
breaking their permeability barriers.

28. Toxins acting on the cell surface: Other pore forming toxins
Toxin
Organism
Activity
Consequence
δ-Hemolysin
S. aureus
Perturbation of the lipid bilayer
Cell permeabilization and lysis
Aerolysin
A. hydrophila
Perturbation of the lipid bilayer
Cell permeabilization and lysis
AT
C. septicum
Perturbation of the lipid bilayer
Cellpermeabilization and lysis

29. Toxins acting on the cell surface:
Insecticidal toxins

The class of insecticidal proteins, also known as
δ-endotoxins, includes a number of toxins produced by
species of Bacillus thuringiensis.

These exert their toxic activity by making pores in the
epithelial cell membrane of the insect midgut.

30. Toxins acting on the cell surface:
Insecticidal toxins

δ-Endotoxins form two multigenic families, cry and cyt;

members of the cry family are toxic to insects of
Lepidoptera, Diptera and Coleoptera orders (Hofmann et al.,
1988),

whereas members of the cyt family are lethal specifically to
the larvae of Dipteran insects (Koni and Ellar, 1994).
Lepidoptera is a large order of insects that includes moths and butterflies.
True flies are insects of the order Diptera.
Coleoptera is an order of insects commonly called beetles.

31. Toxins acting on the cell surface: Insecticidal toxins
Toxin
Organism
Activity
Consequence
PA
B. anthracis
Perturbation of the lipid bilayer
Cell permeabilization and lysis
HlyE
E. coli
Perturbation of the lipid bilayer
Osmotic lysis of cells lining the Midgut
CryIA, CryIIA,
CryIIIA, etc
Bacillus thuringiensis
Destruction of the transmembrane
Potential
Osmotic lysis of cells lining the Midgut
CytA, CytB
B. thuringiensis
Destruction of the transmembrane
Potential
Osmotic lysis of cells lining the Midgut
BT toxin
B. thuringiensis
Destruction of the transmembrane
Potential
Cytocidal activity on human cells

32. Toxins Acting on Intracellular Targets
Class
The group of toxins with an intracellular
Acting on the
target (A/B toxins) contains many toxins
cell surface
with different structures that have only
one general feature in common: they are
Immune system
composed of two domains generally
(Superantigens)
identified as "A" and "B.“
Acting on
intracellular
targets
Injecte
eukaryo
Protein synthesis
Mediators o
Inositol ph
metab
Surface molecules
Signal transduction
Cell membrane
arget

Cytoskeleton structure
Cytoske
Large pore- forming toxins
Intracellular trafficking
Signal tran
Small pore- forming toxins

33. Toxins Acting on Intracellular Targets

The A domain is the active portion of the toxin; it usually
has enzymatic activity and can recognize and modify a
target molecule within the cytosol of eukaryotic cells.

The B domain is usually the carrier for the A subunit; it
bind the receptor on the cell surface and facilitates the
translocation of A across the cytoplasmic membrane.

34. Toxins acting on intracellular targets:
Protein synthesis

These toxins are able to cause rapid cell death at
extremely low concentrations.

This reaction leads to the formation of a completely
inactive EF2-ADP-ribose complex.

35. Toxins acting on intracellular targets:
Protein synthesis

A very important step in the elucidation of the mechanism
of enzymatic activity has been the determination of the
crystal structure for the complex of diphtheria toxin with
NAD.

Upon the addition of NAD to nucleotide-free DT crystals, a
significant structural change.

This change lead to recognition and binding of the
acceptor substrate EF-2.

This would explain why DT recognizes EF-2 only after NAD
has bound.

36. Toxins acting on intracellular targets: Protein synthesis
Toxin
Organism
Activity
Toxins acting on intracellular targets:
Corynebacterium diphtheriae
ADP-ribosylation of EF-2
PAETA P. aeruginosa
Protein synthesis ADP-ribosylation of EF-2
DT
SHT
S. dysenteriae
N-glycosidase activity on 28S RNA
Consequence
Cell death
Cell death
Cell death, apoptosis

37. Toxins acting on intracellular targets:
Signal transduction

Two types of transduction mechanism:

Tyrosine phosphorylation

Modification of a receptor-coupled GTP-binding protein

cyclic AMP

inositol triphosphate

diacylglycerol

38. Pertussis toxin
PT Subunits
A
B

39. Cholera toxin (CT) and E. coli heatlabile enterotoxins (LT-I and LT-II)

Cholera toxin (CT) and E. coli heat-labile enterotoxins (LTI and LT-II) share an identical mechanism of action and
homologous primary and 3D structures.

While V. cholerae exports the CT toxin into the culture
medium, LT remains associated to the outer membrane
bound to lipopolysaccharide.

The corresponding genes of CT and LT are organized in a
bicistronic operon and are located on a filamentous
bacteriophage and on a plasmid, respectively.

40. Clostridium difficile Toxins

Enterotoxin A (TcdA) and cytotoxin B (TcdB) of Clostridium
difficile are the two virulence factors responsible for the
induction of antibiotic-associated diarrhea.

The toxin genes tcdA and tcdB together with three
accessory genes (tcdC-E) constitute the pathogenicity
locus (PaLoc) of C. difficile.

41. Toxins acting on intracellular targets: Signal transduction 1
Toxin
Organism
Activity
Consequence
PT
Bordetella pertussis ADP-ribosylation of Gi
cAMP increase
CT
Vibrio cholerae
ADP-ribosylation of Gi
cAMP increase
LT
E. coli
ADP-ribosylation of Gi
cAMP increase
α-Toxin (PLC)
C. perfringens
Zinc-phospholipase C, hydrolase
Gas gangrene
Toxins A and B (TcdA and
TcdB)
C. difficile
Monoglucosylation of Rho, Rac,
Cdc42
Breakdown of cellular actin
stress fibers
Adenylate cyclase (CyaA)
B. pertussis
Binding to calmodulin ATP→cAMP
conversion
cAMP increase

42. Anthrax Edema and Lethal Factors

The EF and LF genes are located on a large plasmids.

Cleavage of the N-terminal signal peptides yields mature
EF and LF proteins.

LF, is able to cause apoptosis in human endothelial cells.

43. E. coli Cytotoxin Necrotizing Factors and
Bordetella Dermonecrotic Toxin

CNF1 & CNF2: produced by a number of uropathogenic
and neonatal meningitis-causing pathogenic E. coli
strains.

cnf1 is chromosomally encoded, cnf2 is carried on a
large transmissible F-like plasmid called "Vir“.

DNT is a transglutaminase, which causes alteration of
cell morphology, reorganization of stress fibers, and
focal adhesions on a variety of animal models.

44. Cytolethal Distending Toxins

HdCDT is a complex of three proteins (CdtA, CdtB and
CdtC) encoded by three genes that are part of an operon.

Members of this family have been identified in E. coli,
Shigella, Salmonella, Campylobacter, Actinobacillus and
Helicobacter hepaticus.

45. Toxins acting on intracellular targets: Signal transduction 2
Toxin
Organism
Activity
Consequence
Anthrax edema factor (EF)
B. anthracis
Binding to calmodulin ATP→cAMP
conversion
cAMP increase
Anthrax lethal factor (LF)
B. anthracis
Cleavage of MAPKK1 and MAPKK2
Cell death, apoptosis
Cytotoxin necrotizing
factors 1 and 2 (CNF1, 2)
E. coli
Deamidation of Rho, Rac and Cdc42
Ruffling, stress fiber
formation.
DNT
Bordetella species
Transglutaminase, deamidation or
polyamination of Rho GTPase
Ruffling, stress fiber
formation
CDT
Several species
DNA damage, formation of actin
stress fibers via activation of RhoA
Cell-cycle arrest,
cytotoxicity, apoptosis

46. Toxins acting on intracellular targets:
Cytoskeleton structure

The cytoskeleton is a cellular structure that consists of a
fiber network composed of microfilaments, microtubules,
and the intermediate filaments.

It controls a number of essential functions in the
eukaryotic cell:

exo- and endocytosis

vesicle transport

cell-cell contact

and mitosis

47. Toxins acting on intracellular targets:
Cytoskeleton structure

Most of them do it by modifying the regulatory, small G
proteins, such as Ras, Rho, and Cdc42, which control cell
shape.

48. Lymphostatin

Lymphostatin is a very recently identified protein in
enteropathogenic strains of E. coli

Lymphostatin selectively block the production of
interleukin-2, IL-4, IL-5 and γ interferon by human cells
and inhibit proliferation of these cells, thus interfering
with the cellular immune response.

49. Toxins acting on intracellular targets: Cytoskeleton structure
Toxin
Organism
Activity
Toxin C2 and related
proteins
C. botulinum
ADP-ribosylation of monomeric G actin Failure in actin polymerization
Lymphostatin
E. coli
Block of interleukin production
Chronic diarrhea
Block of interleukin production
Chronic diarrhea
Iota toxin and related
C. perfringens
proteins
Consequence

50. Toxins acting on intracellular targets:
Intracellular trafficking

Vesicle structures are essential in:



receptor-mediated endocytosis
and exocytosis
One example of exocytic pathway is that involving the
release of neurotransmitters

51. Mechanism of action of clostridial
neurotoxins (CNT)
Synaptosomal-associated protein 25 (SNAP-25)

52. Helicobacter pylori Vacuolating
Cytotoxin Vac A

This toxin is responsible for massive growth
of vacuoles within epithelial cells.

VacA can insert into membranes forming
hexameric, anion-selective pores.

53. Toxins acting on intracellular targets: Intracellular trafficking
Toxin
Organism
Activity
Consequence
TeNT
C. tetanii
Cleavage of VAMP/ synaptobrevin
Spastic paralysis
BoNT-B, D, G and F
neurotoxins
C. botulinum
Cleavage of VAMP/ synaptobrevin
Flaccid paralysis
BoNT-A, E neurotoxins
C. botulinum
Cleavage of SNAP-25
Flaccid paralysis
BoNT-C neurotoxin
C. botulinum
Cleavage of syntaxin, SNAP-25
Flaccid paralysis
Vacuolating cytotoxin
VacA
H. pylori
Alteration in the endocytic pathway
Vacuole formation,
apoptosis
NAD glycohydrolase
S. pyogenes
Keratinocyte apoptosis
Enhancement of GAS
proliferation

54. Toxins injected into eukaryotic cells

These bacteria intoxicate individual eukaryotic cells by
using a contact-dependent secretion system to inject or
deliver toxic proteins into the cytoplasm of eukaryotic
cells.

This is done by using specialized secretion systems that in
Gram-negative bacteria are called "type III" or "type IV,“.

55. Class
Toxins injected into eukaryotic cells:
Acting on
Acting on the
Mediators of apoptosis: IpaB in Shigella
intracellular

cell surface
targets
Shigella invasion plasmid antigen (Ipa) proteins: IpaA,
Immune
IpaB, IpaC, IpaD. system
Protein synthesis
(Superantigens)
Only IpaB is required to initiate cell death.
Mediators of apoptosis
Surface molecules
Signal transduction
Inositol phosphate
metabolism
Cell membrane
Target

Injected into
eukaryotic cells
Cytoskeleton structure
Cytoskeleton
Large pore- forming toxins
Intracellular trafficking
Signal transduction
Small pore- forming toxins
RTX toxins
Membrane-perturbing
toxins

56. Toxins injected into eukaryotic cells:
Mediators of apoptosis: SipB in Salmonella

An analog of Shigella invasin IpaB.

In contrast to Shigella, Salmonella does not escape from
the phagosome, but it survives and multiplies within the
macrophages.

Salmonella virulence genes are encoded by a chromosomal
operon named sip containing five genes (sipEBCDA).

57. Toxins injected into eukaryotic cells: Mediators of apoptosis
Toxin
Organism
Activity
Consequence
IpaB
Shigella
Binding to ICE
Apoptosis
SipB
Salmonella
Cysteine proteases
Apoptosis
YopP/YopJ
Yersinia species
Cysteine protease, blocks MAPK and NFkappaB pathways
Apoptosis

58. Toxins injected into eukaryotic cells:
Inositol phosphate metabolism

SopB: in Salmonella is homologous to the Shigella flexneri
lpgD virulence factor.

Both proteins contain two regions of sequence similarities
with human inositol polyphosphatases types I and II.

59. Toxins injected into eukaryotic cells: Inositol phosphate metabolism
Toxin
Organism
Activity
Consequence
SopB
Salmonella
species
Inositol phosphate phosphatase, cytoskeleton
rearrangements
Increased chloride
secretion (diarrhea)
IpgD
S. flexneri
Inositol phosphate phosphatase, cytoskeleton
rearrangements
Increased chloride
secretion (diarrhea)

60. Toxins injected into eukaryotic cells: Signal transduction
Toxin
Organism
Activity
Consequence
ExoS
P. aeruginosa
ADP-ribosylation of Ras, Rho GTPase
Collapse of cytoskeleton
C3 exotoxin
C. botulinum
ADP-ribosylation of Rho
Breakdown of cellular actin stress
fibers
ADP-ribosylation of Rho
Modification of actin cytoskeleton
Rac and Cdc42 activation
Membrane ruffling, cytoskeletal
reorganization, proinflammatory
cytokines production
EDIN-A, B and C S. aureus
SopE
S.
typhimurium
SipA
S.
typhimurium
Rac and Cdc42 activation
Membrane ruffling, cytoskeletal
reorganization, proinflammatory
cytokines production
IpaA
Shigella
species
Vinculin binding
Depolymerization of actin filaments
YopE
Yersinia
species
GAP activity towards RhoA, Rac1 or Cdc42
Cytotoxicity, actin depolymerization
YopT
Yersinia
species
Cysteine protease, cleaves RhoA, Rac, and
Cdc42 releasing them from the membrane
Disruption of actin cytoskeleton
VirA
Shigella
flexneri
Inhibition of tubulin polymerization
Microtubule destabilization and
membrane ruffling

61. Toxins injected into eukaryotic cells: Signal transduction
Toxin
Organism
Activity
Consequence
YpkA
Yersinia species
Protein serine/threonine kinase
Inhibition of phagocytosis
YopH
Yersinia species
Tyrosine phosphatase
Inhibition of phagocytosis
Tir
E. coli EPEC
Receptor for intimin
Actin nucleation and pedestalformation
CagA
H. pylori
Tyrosine phosphorylated
Cortactin dephosphorylation
YopM
Yersinia species
Interaction with PRK2 and RSK1 kinases
Cytotoxicity
SptP
S. typhimurium
Inhibition of the MAP kinase pathway
Enhancement of Salmonella capacity to
induce TNF-alpha secretion
ExoU
P. aeruginosa
Lysophospholipase A activity
Lung injury

62. Toxins with unknown mechanism of action
Toxin
Organism
Activity
Consequence
Zot
V. cholerae
?
Modification of intestinal tight junction
permeability
Hemolysin
BL (HBL)
B. cereus
Hemolytic, dermonecrotic and
vascular permeability activities
Food poisoning, fluid accumulation and
diarrhea
BSH
L. monocytogenes ?
Increased bacterial survival and intestinal
colonization

63. Abbreviations
SEA-SEI, staphylococcal enterotoxins
SHT, Shiga toxin;
TSST, toxic shock syndrome toxin
PT, pertussis toxin;
SPE, streptococcal exotoxin
CT, cholera toxin;
SSA, streptococcal superantigen
LT, heat-labile enterotoxin;
SMEZ, streptococcal mitogenic exotoxin z
DNT, dermonecrotic toxin;
MAM, Mycoplasma arthritidis mitogen
CDT, cytolethal distending toxin;
YPMa, Y. pseudotuberculosis-derived mitogen
TeNT, tetanus neurotoxin;
ETA and ETB, exfoliative toxins
RTX, repeats in the structural toxin;
ColH, collagenase
Hly, hemolysin;
Nhe, nonhemolytic entertoxin
Cry, crystal;
PFO, perfringolysin O;
BoNT, botulinum neurotoxin;
SLO, streptolysin O;
Ipa, invasion plasmid antigen;

64. Abbreviations
LLO, listeriolysin O;
Sip, Salmonella invasion protein;
ALO, anthrolisin O;
EDIN, epidermal cell differentiation inhibitor;
AT, α-toxin;
Sop, Salmonella outer protein;
PA, protective antigen;
Ipg, invasion plasmid gene;
DT, diphtheria toxin;
Yop, Yersinia outer protein;
PAETA, Pseudomonas aeruginosa exotoxin A;
GAP, GTPase-activating protein;
GAS, group A Streptococcus;
Vir, virulence protein;
YpkA, Yersinia protein kinase A;
Tir, translocated intimin receptor;
EPEC, enteropathogenic E. coli;
CagA, cytotoxin-associated gene A;
SptP, Salmonella protein tyrosine phosphatase;
VAMP, vesicle-associated membrane protein;
ICE, interleukin-1β-converting enzyme;
SNAP, synaptosome-associated protein;
MAPKK, mitogen-activated protein kinase ;
Zot, zonula. occludens toxin; and BSH, bile salt hydrolase.

65. Enzymatic activities
Glucosyl-transferases
Deamidases
ADP-ribosyltransferases
N-Glycosidases
Metalloproteases

66. Substrate
Effect
DT
ADP-ribosyltransferases
Toxin
Elongation factor EF-2
Cell death
PAETA
Elongation factor EF-2
Cell death
PT
Gi, Go and transducin
cAMP increase
CT
Gs, Gt and Golf
E. coli LT
Clostridium botulinum C2
Actin
Failure in actin
P. aeruginosa ExoS
Ras
Collapse of cytoskeleton
Clostridium botulinum C3
Rho
Breakdown of cellular actin stress
fibers

67. Toxin
Effect
Clostridium difficile toxins A and B
Rho/Ras GTPases
Breakdown of cytoskeletal structure
E. coli CNF1
Glucosyl-transferases
Substrate
Rho, Rac and CdC42
Stress fiber formation
Deamidases
Bordetella DNT
Metalloproteases
Shiga toxin
Ribosomal RNA
Stop of protein synthesis
Bacillus anthracis LF
N-Glycosidases
Rho,
Macrophages
Disruption of normal homoeostatic
functions
Clostridium tetanii TeNT
VAMP/synaptobrevin
Spastic paralysis
C. botulinum BoNTs
VAMP/synaptobrevin, SNAP-25
Flaccid paralysis

68. Abbreviations
SNAP-25, synaptosome-associated protein of 25 kDa.
CNF1, cytotoxin necrotizing factor 1;
DNT, dermonecrotic factor;
DT, diphtheria toxin;
PAETA, Pseudomonas aeruginosa exotoxin A;
PT, pertussis toxin;
CT, cholera toxin;
LT, heat-labile enterotoxin;
ExoS, exoenzyme S;
LF, lethal factor;
TeNT, tetanus neurotoxin;
BoNT, botulinum neurotoxin;
VAMP, vesicle associated membrane protein;

69. Thank You