Influence of Different Antigen Administrations on the Production of
Antibodies against Clostridium perfringens Beta Toxin
Yiwen Zhu
Vista Del Lago High School, Folsom, California 95630, U.S.A.
Keywords: Intermuscular, Intraperitoneal, Intradermal, DNA Vaccine, Homogenous Boost.
Abstract: Clostridium perfringens beta toxin (CPB) is a toxin produced by C.perfringens that is responsible for
hypertension and necrotic enteritis in mammals. Currently, DNA vaccines have been implemented to avoid
such toxins. Previous studies have shown that heterologous prime boosting helps with the identification of
CPB by producing more antibodies. However, there was no suggestion that differences in the administration
of antibodies can further influence the production of antibodies. The study focuses on the optimal injection
administration of DNA vaccine and the heterologous protein boost targeting CPB. The study provides
important information to maximize the efficiency of immune response against CPB from the vaccine for
mammals.
1 INTRODUCTION
Th1 and Th2 cells are two types of T helper cells
which leads to an increase in cell-mediated response
against virus, bacteria, and other possible pathogens
(Kidd 2003). Specifically, Th1 cells produce
interferon-gamma, interleukin -2, and tumor necrosis
factor (TNF). Th2 cells produce IL-4, IL-5, IL-10, IL-
13 (Romagnani 1999). These cytokines are
responsible for a strong antibody production and the
activation of eosinophil. These two immune cells are
essential to the adaptive immune system to carry out
its goal in fighting off infections.
Clostridium perfringens beta toxin (CPB) is
responsible for necrotic enteritis, a disease that can be
seen on humans after consuming unclean meat, in
mammals and causes hypertension. It is one of the
four major toxins produced by Clostridium
perfringens. Recent studies have shown that by using
a heterologous prime-boosting strategy in the DNA
vaccine, the amount of anti-rCPB antibody response
was stronger in comparison to a homologous boosting
strategy. Heterologous strategy triggers both Th1 and
Th2 response and the balance in response was
necessary for the success of the vaccine. A possible
link to the success is the increase in both levels of
IgG1 and IgG2b antibodies in comparison to the
IgG2b only reaction in homologous boosting
response. However, there was no evidence suggesting
that the administration of antigens influences the
immune response by resulting in a better
identification and neutralization of the toxin (Solanki,
A. K., Bhatia, B., Kaushik, H., Deshmukh, S. K.,
Dixit, A., & Garg, L. C. 2017). Previous study has
shown that Th1 and Th2 immune responses are not
strictly synchronized because Th2 immune responses
suppress the activities of phagocytosis. Under the
infection of large eukaryotic pathogens, Th1 cell
response can be seen as protective and Th2 cell
response would resolve the inflammation
(Romagnani 1999).
There are seven discovered routes which antigen
administration has in the humoral immune response:
intravenous, intraperitoneal, intermuscular,
intranodal, intrasplenic, intradermal, and
subcutaneous. This study will focus on
intraperitoneal, intermuscular, and intradermal
routes. Previous study suggests that different antigen
administrations have no significant influence on
antibody production. I hypothesize that the
introduction of vaccine into the host of clostridium
perfringens beta toxin will result in most
improvement in the production of antibodies
measured by ELISA and a better identification and
neutralization of the toxin after immunization
through the intradermal, following intramuscular, and
lastly intraperitoneal.
716
Zhu, Y.
Influence of Different Antigen Administrations on the Production of Antibodies against Clostridium perfringens Beta Toxin.
DOI: 10.5220/0011263800003443
In Proceedings of the 4th International Conference on Biomedical Engineering and Bioinformatics (ICBEB 2022), pages 716-722
ISBN: 978-989-758-595-1
Copyright
c
2022 by SCITEPRESS – Science and Technology Publications, Lda. All rights reserved
2 MATERIALS
2.1 Cells Used in the Study
E. coli DH5α and BL21 pLysS cells were used in the
study along with DNA information and modifying
enzymes.
2.2 Genetic Information of the CPB
Genetic information of the beta toxin in this study
was used to optimize reactions. Genetic information
will also be later used to introduce the booster shot in
all mices. In order to fit the large requirements in this
study. This piece of genetic information will be
replicated through the process of PCR.
2.3 ELISA (Enzyme-Linked
Immunosorbent Assay)
The antigen-specific antibodies of each group will be
read by ELISA. In the study the antibody will be
specific to Anti-rCPB antibodies.
2.4 Mice Immunization
In this study, each experimental group will contain 3
mice. Each mice will be immunized with 100ug of
plasmid DNA following a booster shot of rCPB on
day 15 after immunization. There will be a total of 29
groups of mice in this study to examine specific
differences. They will be the 27 possible results
presented by the different combinations of antigen
administrations along with positive control group and
negative control group. The positive control group
will receive the inactivated bacteria. In addition, the
negative control group will receive saline at all
routes.
2.5 Data Analysis
Significance of all levels of antibody production
measured by ELISA will be analyzed on TI-84 Plus
CE. (p<0.05)
3 RESULTS
Possible results on the production of antibodies for
different antigen administrations. All 27 possible
results can be seen at Table 1 Different Antibody
Production Measured by ELISA.
3.1 Possible Result #1
DNA vaccine administered through the
intramuscular route, receiving the booster shot
through the same route. The production of
antibodies in these specific combinations will not
produce any antibodies against CPB.
3.2 Possible Result #2
DNA vaccine administered through the
intradermal route, receiving the booster shot
through the same route. The production of
antibodies in these specific combinations will not
produce any antibodies against CPB.
3.3 Possible Result #3
DNA vaccine administered through the
intraperitoneal route, receiving the booster shot
through the same route. The production of
antibodies in these specific combinations will not
produce any antibodies against CPB.
3.4 Possible Result #4
DNA vaccine administered through the
intramuscular route, receiving booster shot
through the intradermal route. The production of
antibodies in these specific combinations will not
produce any antibodies against CPB.
3.5 Possible Result #5
DNA vaccine administered through the
intramuscular route, receiving the booster shot
through the intraperitoneal route. The production
of antibodies in these specific combinations will not
produce any antibodies against CPB.
3.6 Possible Result #6
DNA vaccine administered through the
intraperitoneal route, receiving the booster shot
through the intramuscular route. The production
of antibodies in these specific combinations will not
produce any antibodies against CPB.
3.7 Possible Result #7
DNA vaccine administered through the
intraperitoneal route, receiving the booster shot
through the intradermal route. The production of
antibodies in these specific combinations will not
Influence of Different Antigen Administrations on the Production of Antibodies against Clostridium perfringens Beta Toxin
717
produce any antibodies against CPB.
3.8 Possible Result #8
DNA vaccine administered through the
intradermal route, receiving the booster shot
through the intramuscular route. The production
of antibodies in these specific combinations will not
produce any antibodies against CPB.
3.9 Possible Result #9
DNA vaccine administered through the
intradermal route, receiving the booster shot
through the intraperitoneal route. The production
of antibodies in these specific combinations will not
produce any antibodies against CPB.
3.10 Possible Result #10
DNA vaccine administered through the
intramuscular route, receiving the booster shot
through the same route. The production of
antibodies in these specific combinations will
produce high enough antibodies against CPB to
efficiently eliminate the bacteria.
3.11 Possible Result #11
DNA vaccine administered through the
intradermal route, receiving the booster shot
through the same route. The production of
antibodies in these specific combinations will
produce high enough antibodies against CPB to
efficiently eliminate the bacteria.
3.12 Possible Result #12
DNA vaccine administered through the
intraperitoneal route, receiving the booster shot
through the same route. The production of
antibodies in these specific combinations will
produce high enough antibodies against CPB to
efficiently eliminate the bacteria.
3.13 Possible Result #13
DNA vaccine administered through the
intramuscular route, receiving booster shot
through the intradermal route. The production of
antibodies in these specific combinations will
produce high enough antibodies against CPB to
efficiently eliminate the bacteria.
3.14 Possible Result #14
DNA vaccine administered through the
intramuscular route, receiving the booster shot
through the intraperitoneal route. The production
of antibodies in these specific combinations will
produce high enough antibodies against CPB to
efficiently eliminate the bacteria.
3.15 Possible Result #15
DNA vaccine administered through the
intraperitoneal route, receiving the booster shot
through the intramuscular route. The production
of antibodies in these specific combinations will
produce high enough antibodies against CPB to
efficiently eliminate the bacteria.
3.16 Possible Result #16
DNA vaccine administered through the
intraperitoneal route, receiving the booster shot
through the intradermal route. The production of
antibodies in these specific combinations will
produce high enough antibodies against CPB to
efficiently eliminate the bacteria.
3.17 Possible Result #17
DNA vaccine administered through the
intradermal route, receiving the booster shot
through the intramuscular route. The production
of antibodies in these specific combinations will
produce high enough antibodies against CPB to
efficiently eliminate the bacteria.
3.18 Possible Result #18
DNA vaccine administered through the
intradermal route, receiving the booster shot
through the intraperitoneal route. The production
of antibodies in these specific combinations will
produce high enough antibodies against CPB to
efficiently eliminate the bacteria.
3.19 Possible Result #19
DNA vaccine administered through the
intramuscular route, receiving the booster shot
through the same route. The production of
antibodies in these specific combinations will
produce a low amount of antibodies against CPB that
doesn’t support an efficient response to eliminate the
bacteria.
ICBEB 2022 - The International Conference on Biomedical Engineering and Bioinformatics
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3.20 Possible Result #20
DNA vaccine administered through the
intradermal route, receiving the booster shot
through the same route. The production of
antibodies in these specific combinations will
produce a low amount of antibodies against CPB that
doesn’t support an efficient response to eliminate the
bacteria.
3.21 Possible Result #21
DNA vaccine administered through the
intraperitoneal route, receiving the booster shot
through the same route. The production of
antibodies in these specific combinations will
produce a low amount of antibodies against CPB that
doesn’t support an efficient response to eliminate the
bacteria.
3.22 Possible Result #22
DNA vaccine administered through the
intramuscular route, receiving booster shot
through the intradermal route. The production of
antibodies in these specific combinations will
produce a low amount of antibodies against CPB that
doesn’t support an efficient response to eliminate the
bacteria.
3.23 Possible Result #23
DNA vaccine administered through the
intramuscular route, receiving the booster shot
through the intraperitoneal route. The production
of antibodies in these specific combinations will
produce a low amount of antibodies against CPB that
doesn’t support an efficient response to eliminate the
bacteria.
3.24 Possible Result #24
DNA vaccine administered through the
intraperitoneal route, receiving the booster shot
through the intramuscular route. The production
of antibodies in these specific combinations will
produce a low amount of antibodies against CPB that
doesn’t support an efficient response to eliminate the
bacteria.
3.25 Possible Result #25
DNA vaccine administered through the
intraperitoneal route, receiving the booster shot
through the intradermal route. The production of
antibodies in these specific combinations will
produce a low amount of antibodies against CPB that
doesn’t support an efficient response to eliminate the
bacteria.
3.26 Possible Result #26
DNA vaccine administered through the
intradermal route, receiving the booster shot
through the intramuscular route. The production
of antibodies in these specific combinations will
produce a low amount of antibodies against CPB that
doesn’t support an efficient response to eliminate the
bacteria.
3.27 Possible Result #27
DNA vaccine administered through the
intradermal route, receiving the booster shot
through the intraperitoneal route. The production
of antibodies in these specific combinations will
produce a low amount of antibodies against CPB that
doesn’t support an efficient response to eliminate the
bacteria.
Influence of Different Antigen Administrations on the Production of Antibodies against Clostridium perfringens Beta Toxin
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Table 1 Different Antibody Production Measured by ELISA
4 DISCUSSION
Previous studies have shown that there would be an
increase in immune response when an extra booster
shot is injected in addition to the shot of DNA vaccine
targeting CPB. This study applied the ELISA method
to examine how the production of antibodies can be
influenced by different methods of administration.
The hypothesis made for this experiment is based on
a logical assumption. Intradermal injection is not
common for vaccination because it requires a difficult
technique which slows down the efficiency to
vaccinate the population. However, areas of
intradermal injection generally contain large amounts
of dendritic cells, which are immune cells that present
antigens to the adaptive immune system, where
antibodies are produced. However, with livestock
vaccination, it would be more ideal than
intramuscular injection since some mammals have a
thick skin layer. Therefore, I hypothesize that
intradermal would be the most effective out of the
three routes. Intermuscular, or the injection of
vaccine in the muscle, is predicted to have less
antibody production when compared to intradermal
injection because muscles have more blood supplies
which indicates that as cytokines are released, it will
be easier for neutrophils to reach the site of injection
and process the materials injected into the muscles
and absorb the information. The least effective
method of three would be intraperitoneal for various
reasons. This injection method is largely used in mice
rather than humans or larger cattles since larger
mammals would require a larger needle to be able to
ICBEB 2022 - The International Conference on Biomedical Engineering and Bioinformatics
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reach the abdomen. In addition, this injection route is
usually for a large concentration of fluid which is not
a typical feature of vaccines. Booster injections may
also play a role in the production of antibodies. Since
the immune system would already have memories of
CPB after the injection of the vaccine, it would be the
same logic as the initial exposure to antigen, placing
the injection site at a location with easier absorption
and presentation of antigens would result in the most
production of antibodies.
The possible results that are provided by Table 1.
It presents three different possible results in the
production of antibodies for a specific injection
combination. When there are no antibodies produced,
the possible explanation is that the specific injection
site doesn’t trigger the immune system at all.
Previous studies proved that the DNA Vaccine would
trigger an immune response and produce specific
antibodies against the toxin (Solanki, A. K., Bhatia,
B., Kaushik, H., Deshmukh, S. K., Dixit, A., & Garg,
L. C. 2017). However, if the method did not produce
any antibodies for all mice in a group with the same
route for both the injection of booster protein and
vaccine, it signifies that the route somehow does not
trigger an immune response inside the mice, meaning
that the immune cells involved in the innate immune
response does not recognize any pathogen and
thereby not presenting any antigen for the production
of antibodies. I believe that such a situation is not
likely. However, there is no evidence to prove the
nonexistence of such possibility nor evidence of the
principle behind the observation.
When looking at the result, the results of mice
groups of the two routes that are identical to each of
the pathways should be compared. For instance, the
results of possible result #14 presents two different
routes: intramuscular and intraperitoneal. Hence the
production of antibodies of result #1 and 3 should be
compared with result #14. If both of them function
properly, this data signifies that the route of injection
is able to effectively trigger an immune response as
protein or vaccine is injected at the site.
On the other hand, it would be obvious that there
are other factors contributing to the lack of antibodies
produced. Similar to the first observation, such a
result is unlikely to occur. There is also the possibility
that no antibody binded to the plate in ELISA.
However, since there are multiple serums of mice
being tested, it is quite unlikely that no antibody
attached to any of the receptors in the plates.
Other possible observations of the presence of
produced antibodies against CPB are much more
likely to occur in reality. If a general trend is
discovered in the difference between each
combination of antigen administrations, specifically
the difference between a high production and a low
production, it is possible that the observation is a
result of the efficient connection between the antigen
receiving B cells and the activated B cells that are
responsible for the production of antibodies.
However, each mammal may have different features
of the immune system. It is not possible to test an
individual mammal multiple times on the specific
vaccines since the immune system would already
have memory of the antigen. Therefore, antibody
production using a separate vaccine on the same
mammal can be observed to discover if the low
production of anti-CPB is a result of ineffective
delivery of antigen information or of injection sites.
5 CONCLUSION
This study explores the influences of different
injection administration on the production of
antibodies against Clostridium perfringens beta toxin.
It is predicted that intradermal injection will produce
the most amount of antibodies, followed by
intramuscular injection having the second most
production and intraperitoneal being the least
effective. The possible results predict the potential
relationship between the identification of antigen
after initial injection and the delivery of information
in the immune system. Since the hypothesis made in
this study can only be directly supported or rejected
with numbers, Table 1 suggests that results #1, 3, 5,
6, 11, 13, 16, 17, 18, 19, 21, 23, and 24 all partially
support the hypothesis and #2, 4, 7, 8. 9. 10. 12. 14,
15, 20, 22, 25, 26, 27 all partially rejected the
hypothesis. In addition, since the use of DNA vaccine
has been prevalent on livestock to prevent economic
losses, the result of the study will be able to advance
the efficiency of vaccination. However, since there
are more than three injection administrations and
different animals support different injection methods,
further comparison between all the routes is
necessary before concluding the most efficient
method for the vaccination of Clostridium
perfringens beta toxin on different mammal species.
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