use of bacteria in cancer therapy

Question 1

A cancer

Answer 1

can be metastatic, invasive, malignant and agressive

it is a general term that refers to a group of disease characterized by growth and spread of abnormal growth

Question 1

a tumour

Answer 1

can be benign or malignant. Abnormal growth of tissue
It is defined by a solid mass, a neoplasm that does not invade or does surrounding tissues

malignant tumors

Question 2

a neoplasm

Answer 2

are cells that starts to grow abnormally. Can be benign or malignant but they start to proliferate

it is every abnormal proliferation of genetically altered cells benign or malignant

Question 3

carcinoma

Answer 3

affect skin, colon or lung. They are abnormally of ectodermal and endodermal tie-ssues

Question 4

sarcoma

Answer 4

abnormalities of mesodermal tissues such as blood vessels, bone, fat.

Question 5

helicobacter as causative agent

Answer 5

chronic infection can cause MALT lymphoma y increase acid production. Can also cause Gastric cancer by increasing acid productions though dysplasia and ulcer formation
Bacteria can promote carcinogenesis

Question 6

Bacterial DNA

Answer 6

bacteria are richer in CpG unmethylated sequence, whay more than mammalian. These are detected as PAMPS by TLR on B cell and dendritic cells.

This TLR9 activation leads to a strong cytotoxic T CELL response and help to bypass the tumor induced suppression of the immune system

In B cells, it lease to the production go IL6, 12 and chemokine, as well as IgM production.
in DC, the expression of MHC is enhanced, which increase IL1,6? 12, 18 and TNF production, as well as increase APC function, which activate T helper cells.

CD4 cells than can activate CTL cell, produce interferon gamma and B cell leads the adaptive immunity with IgG production.

These bacteria DNA is used to boost the tumor antigen recognition by the immune system.

drawbacks include the fact that it is hard to purify CpG rich bacterial DNA for human application because of LPS contamination (toxins causing fever), bacterial DNA tend to be degraded by human nucleases and it is hard to engineer them to directly target the tumors.

The solutions at the moments are the production of nuclease resistance synthetic CpG oligodeoxynucleotides (ODN) to counteract LPS contamination. Improved uptake by self assembled nonmaterial CpG ODN complexes

Question 7

bacterial toxins
A) toxins to target receptor directly

Answer 7

A) toxins to target receptor directly
Clostridium perfringens can produce an enterotoxins which is release in small intestins and bind to epithelial cells. It usually cause food poisoning. It works by directed binding to cell via a tight junction proteins, which causes conformational changes and pore like structure creating change in the membrane permeability.

As anti tumoral agents, it would be use to change the cell permeability, causing osmotic imbalance in tumor cells and therefore cytolysis.

They recurrently working on recombinant CPE that could be combine to therapeutic proteins or drug loaded nanoparticles.
However, the tumor specificity is not clear yet. This is because CPE receptor are over expressed in a lot of different cancer ok ok but also a low level in healthy cells which could lead to a systemic toxicity.
It limits its use but For example could be used in brain metastases cause CPE receptor is absent in normal brain tissue

Question 8

bacterial toxins
b) immunotoxins: ligand bound toxins

Answer 8

basically it is an adaptations of the toxins. they use for example the diphtheria toxins or the pseudomonas toxins which are both AB toxins and both bind to a lot of receptors in many cell type! For tumor treatment these AB toxins can be exploited by removing the receptor binding domain and replace it by a ligand that could directly target the tumor receptor. By this you gain specificity and keep the cytotoxins effect.

Question 9

bacterial toxins
c) superantigens

Answer 9

super antigens are not produced by APC.
They are functional molecules which do not require further processing and that can directly bind to MHC class 2 molecular of APC. The MHC super AG complex can then directly interact with TCR and it boost it so much it can give sepsis!! It can activate up to 20% of T cells, release loads of cytokines and disturb the normal immune response.

loads of bacterial toxins can act as super AG, it gives an advantage as it allow to evade the immune system and prolong survival by causing a local inflammation and therefore they get plenty of blood and nutrient.

For tumeurs targeted superantigens (TTS), the idea would be to induce a strong and local cytotoxic T cell attach that would kill the tumor cells and produce inflammation. This can be done by using recombinant super antigens. The super antigens would be mutated by linking it to a Fab or a monoclonal antibody that is directly targeted against a tumor antigens.

Exemple:naptumomab estafenatox: the modified enterotoxins is fused to FAB which recognized the 5T4 antigens . 5T4 is expressed in a lot of cancer but not on normal tissues; so the FAB bind to it, then the toxins aka Super AG allow binding to MHC2 (increase safety profile), which activate the T lymphocyte and allow direct killing.

Question 10

bacterial toxins:
d) anti-tumor antibiotics

Answer 10

super important chemotherapeutics. They have a lot of MOA such as DNA intercalation, inhibition of RNA transcription, preventing the protein synthesis, etc

exemples:
Azurin is secreted by pseudomonas aeruginosa. It has a Cu-containing electron transfer protein and allow it to preferentially penetrate cancer cells. It leads to a complex formation with p 53 (tumor suppressor protein), leading to increase p53 concentration which causes cell shrinkage and death through apoptosis and growth arrest. +++ inhibit the tumor angiogenesis. BUUUT the question of tumor specificity is not entirely answered.

Question 11

limitation of bacterial products

Answer 11

the MOA is not always well understood. There is still work done to diminish toxicity and enhance the specificity.

the numbers will increase thanks to the development in combinatorial bio synthesis and the advancement in meta genomic.

Question 12

live bacteria in cancer therapy

Answer 12

3 approaches can be taken

either bacteria is a vector for protein transfer to the tumor site
or
the bacteria is an immune adjuvant to evoke the immune repose indirectly
or
the bacteria is used as a DNA/protein vaccine to target the cancer

Question 13

live bacteria as a protein transfer system - Clostridium

Answer 13

a) can be used to target tumor colonization with obligate anaerobic bacteria. You use the tumor hypoxia to bring and produce your proteins to attack the tumor cells

b) same by using facultative anaerobic bacteria. These are auxotrophic strains that would benefit of the tumor micro environnement.

example: Clostridium (anaerobic obligate bacteria: endospore formation))
in the 1900 it was used for cancer treatment as it was shown that colonisation was restricted to the tumors, released bacterials proteins and destroyed large tumors parts. However, the outer rime of the viables cells seemed to persist and the oncolysis ofter led to tumor lysis syndrome . So basically it was killing the tumor from inside but not the outside.
in A99(, an attenuated stain was used (deletion of a lethal gene) that seem to spread extensively throughout the tumor. It had great oncolytic properties as it produced enzyme that attacked the tumor cells and causing enlargement of necrotic regions. It was also causing a strong immune response. It was a good balance but the outer viable rime problem was not solved. The solution for this was COBALT: combination bacteriolytic therapy which combined the use of C. novyi NT treatment and radio/chemotherapy. So C. novae NT and Doxil (liposome encapsulated doxorubicin) was given and let to a great survival rate.

other non pathogenic recombinant clostridium can be used such as proteolytic clostridia or recombinantly ended with therapeutic gene clostridium. This is called CDEPT: clostridium directed enzyme prodrug therapy. the enzyme of the bacteria convert the produce, leading to the production of targeted cytotoxic, immune modulation or anti vascular proteins at the site of action wanted. The use of c novae in combination actually allow to reduce conventional therapy level .

Question 14

live bacteria as protein transfer system - Salmonella

Answer 14

• Salmonella Typhimurium Prine mutant (need external purine sources - auxotrophs): You gain tumors specificity based on the excessive presence of purine the in necrotic area of the tumor regions. In this case, recombinant strain are often used - Tumour amplified protein expression therapy (TAPET)
• Salmonella typhimurium A1-R (leu-arg auxotroph): need tumor tissue to survive.

Question 15

live bacteria as adjuvant in cancer immunotherapy

Answer 15

use of Basil Calmette Guérin, it is an attenuated Mycobacterium Boris strain. It is used as live vaccine against tuberculosis and leprosys.

It is used in bladder cancer treatment! the patient lie down and the compound get active in the bladder (not fully understood).
BCG get attached to urothelial tumor cells through fibronectin attachement protein (critical step), it get internalized by the cells and it is then believed that BCG itself create a cytotoxic effect on the cells. In addition, it seems that BCG uptake evoke the ignition of an immune response which is strong and local. This can e done through antigen presenting and cytokine release by bladder cells, leading to MHC1 up regulation, ICAM-1 and multiple chemoattractant proteins release. This leads to immune recruitment

the efficacy of this therapy is based on the long lasting local immune activation : by the cytokine and chemokine, by the BAK ( BCG activated killer) cell generation AND the proaction of the performs by the BAK cells.

current problems with this are the toxic side effect by the extensive inflammation, high level of recurrent, the different reaction profile and the limited understanding of the antitumour effect.

Improvement of the BCG therapy could be done by the use of.a lower toxic strain, a recombinant mycobacterium Boris strain that would produce cytokines specific, and other. however, we still dont know how an individual could react.

Question 16

live bacteria as cancer vaccine

Answer 16

Live or attenuated bacteria are used as vectors to transfer gene or proteins of interest to APC, which results in an anti-tumor immunoreaction.

different bacteria have been studies for this purpose. However some cannot be use in pregnant women because at risk of meningitis.

gene or proteins of interest can include tumor specific or associated antigens that are very specific to these tumor cells. In addition, it could be gene or proteins involved in the tumor angiogenesis.

Tumor specific antigens (ne-antigens) are specific to 1 tumor cell type that have mutation from a gene.

Tumor associated antigens can be present on more tumor cell types and are generally overexpresse, oncofoetal protein are proteins derived from oncoviruse. (these are better).

A live bacterium can enter into a cells via phagocytosis, pinocytosis or receptor mediated endocytosis. The vaccination via DNA or protein then happens through release into the APC

or it is directly injected in the cells through the bacterial secretion machinery.

DNA vaccine: a plasmid construct that carries a prokaryotic gene needed for plasmid replication in bacterium. AND an eukaryotic caused with the transcription translation signals so the gene of interest can be placed under control of the eukaryotic signals.

PROTEIN vaccine: the protein here is directly produced by the bacteria so you definitely need prokaryotic secretion. You usually get a better vaccination by secreted AG. protein, you can exploite several secretion pathway to secrete the recombinant protein. However, the effect is protein level dependent. So it can be hard to predict.

Question 17

secretion pathways:
Type 1 or ABC

Answer 17

secretion pathways:
Type 1 or ABC: the apparatus is made of the ABC export protein, the membrane fusion protein and the outer membrane protein. the C terminal secretion signal is recognized by the protein of interest and get transported

Question 18

secretion pathways: Type III (TTSS) secretion system

Answer 18

it is activated in contact with the host cell and protein injection into cells.

fusion of YOP (yersinia outer protein) effector part with the protein of interest which leads to the protein translocation into the host.

Question 19

seèretione pathway: type 5 autotransporter secretion.

Answer 19

1 proteins which contain 3 domains
an N terminal signal sequence, a mature secreted protein (passenger domain) and a c terminal forming the POREin the outer membrane.

you can replace the passenger domain by the protein of interest

gram + are less complicated because they only have one layerfun

Question 20

Live bacteria as vaccine: functionalisation of live bacteria

Answer 20

nanoBEADS (nanoscale bacterium enabled autonomous drug delivery system)

the bacteria at the cell surface is loaded with nanoparticles carrying the DNA or proteins. You dont need genetic modification and it leads to an accurate delivery and controllable release of the load. the nanoparticle is negative while bacteria +

Question 21

live bacteria - and +

Answer 21

**advantage: **
For DNA vaccination, the possibility of post translational modification allow to target conformationally restricted epitopes.
The cost and labour is low as bacterial carrier strain are easy to manufacture, cheap and fast
you dont need purification step in contrast to naked DNA vaccine
most carrier bacteria allow for mucosal immunisation through oral route
the bacteria cell wall is plenty of epitope eg PAMPS which allow for a better activation of the immune system

disadvantage include the fact that live bacteria can have an unpredictable efficacy. Although attenuated, immunocompromised person can have bad side effect
CpG related toxicity is present

Question 22

recent development

Answer 22

outer membrane vesicles as cancer vaccine to enhance immunity response, and avoid pathogenicity.
Improvement of bacterial cancer therapy using syntethic biology allow to optimise the combination of best working element

nano beads have been used to activate functionalism bacteria with in vitro signal.

Question 23

hypoxia as cause of INTRINSIC resisitance

Answer 23

hypoxic cells are not reached by chemo or radiation. Usually, chemotherapeutic target well proliferating cells

a solution can be hypoxic activated prodrugs

Question 24

hypoxia as cause of MOLECULAR resistance

Answer 24

cancerous cells have adopted an hypoxia tolerance
therefore viable cells that are hypoxic exist inside tumor regions.
They developed this by genetic and metabolism changes in tumor cells that regulate multiple pathways such as the hypoxia inducible factor pathway

this results in a more malignant phenotype due to high metastasis, induction of Neo-angigenesis, and selection of cells with diminished apoptotic potential, which increase therapy resistance