The document discusses the immune system and its defenses against pathogens. It describes three lines of defense: first being physical and chemical barriers like skin and mucus, second being the inflammatory response, and third being the adaptive immune system involving B and T lymphocytes and antibodies. It provides details on lymphocytes, antibodies, antigens, active and passive immunity, and the roles of the humoral and cell-mediated immune responses.
Non-Specific Immune Response, Innate immunity, inherent immunity, Role in overall immunity of individual, Significance, components involve in Non-Specific Immune Response,
Immune system is our defense mechanism which provides protection against various infections and ailments. Low immunity is the root cause for all the problems so Planet Ayurveda presents a fabulous herbal formulation for enhancing immunity power.
Immunity can be defined as a complex biological system endowed with the capacity to recognize and tolerate whatever belongs to the self, and to recognize and reject what is foreign.
Non-Specific Immune Response, Innate immunity, inherent immunity, Role in overall immunity of individual, Significance, components involve in Non-Specific Immune Response,
Immune system is our defense mechanism which provides protection against various infections and ailments. Low immunity is the root cause for all the problems so Planet Ayurveda presents a fabulous herbal formulation for enhancing immunity power.
Immunity can be defined as a complex biological system endowed with the capacity to recognize and tolerate whatever belongs to the self, and to recognize and reject what is foreign.
IMMUNITY:
INTRODUCTION:
Our immune system is essential for our survival.
Without an immune system, our bodies would be open to attack from bacteria, viruses, parasites, and more.
It is our immune system that keeps us healthy as we drift through a sea of pathogens.
The human body has a special design, it protects itself against any invaders. In this presentation you will learn about the self defense mechanisms of the body.
GDG Cloud Southlake #33: Boule & Rebala: Effective AppSec in SDLC using Deplo...James Anderson
Effective Application Security in Software Delivery lifecycle using Deployment Firewall and DBOM
The modern software delivery process (or the CI/CD process) includes many tools, distributed teams, open-source code, and cloud platforms. Constant focus on speed to release software to market, along with the traditional slow and manual security checks has caused gaps in continuous security as an important piece in the software supply chain. Today organizations feel more susceptible to external and internal cyber threats due to the vast attack surface in their applications supply chain and the lack of end-to-end governance and risk management.
The software team must secure its software delivery process to avoid vulnerability and security breaches. This needs to be achieved with existing tool chains and without extensive rework of the delivery processes. This talk will present strategies and techniques for providing visibility into the true risk of the existing vulnerabilities, preventing the introduction of security issues in the software, resolving vulnerabilities in production environments quickly, and capturing the deployment bill of materials (DBOM).
Speakers:
Bob Boule
Robert Boule is a technology enthusiast with PASSION for technology and making things work along with a knack for helping others understand how things work. He comes with around 20 years of solution engineering experience in application security, software continuous delivery, and SaaS platforms. He is known for his dynamic presentations in CI/CD and application security integrated in software delivery lifecycle.
Gopinath Rebala
Gopinath Rebala is the CTO of OpsMx, where he has overall responsibility for the machine learning and data processing architectures for Secure Software Delivery. Gopi also has a strong connection with our customers, leading design and architecture for strategic implementations. Gopi is a frequent speaker and well-known leader in continuous delivery and integrating security into software delivery.
Let's dive deeper into the world of ODC! Ricardo Alves (OutSystems) will join us to tell all about the new Data Fabric. After that, Sezen de Bruijn (OutSystems) will get into the details on how to best design a sturdy architecture within ODC.
Smart TV Buyer Insights Survey 2024 by 91mobiles.pdf91mobiles
91mobiles recently conducted a Smart TV Buyer Insights Survey in which we asked over 3,000 respondents about the TV they own, aspects they look at on a new TV, and their TV buying preferences.
DevOps and Testing slides at DASA ConnectKari Kakkonen
My and Rik Marselis slides at 30.5.2024 DASA Connect conference. We discuss about what is testing, then what is agile testing and finally what is Testing in DevOps. Finally we had lovely workshop with the participants trying to find out different ways to think about quality and testing in different parts of the DevOps infinity loop.
JMeter webinar - integration with InfluxDB and GrafanaRTTS
Watch this recorded webinar about real-time monitoring of application performance. See how to integrate Apache JMeter, the open-source leader in performance testing, with InfluxDB, the open-source time-series database, and Grafana, the open-source analytics and visualization application.
In this webinar, we will review the benefits of leveraging InfluxDB and Grafana when executing load tests and demonstrate how these tools are used to visualize performance metrics.
Length: 30 minutes
Session Overview
-------------------------------------------
During this webinar, we will cover the following topics while demonstrating the integrations of JMeter, InfluxDB and Grafana:
- What out-of-the-box solutions are available for real-time monitoring JMeter tests?
- What are the benefits of integrating InfluxDB and Grafana into the load testing stack?
- Which features are provided by Grafana?
- Demonstration of InfluxDB and Grafana using a practice web application
To view the webinar recording, go to:
https://www.rttsweb.com/jmeter-integration-webinar
Builder.ai Founder Sachin Dev Duggal's Strategic Approach to Create an Innova...Ramesh Iyer
In today's fast-changing business world, Companies that adapt and embrace new ideas often need help to keep up with the competition. However, fostering a culture of innovation takes much work. It takes vision, leadership and willingness to take risks in the right proportion. Sachin Dev Duggal, co-founder of Builder.ai, has perfected the art of this balance, creating a company culture where creativity and growth are nurtured at each stage.
Key Trends Shaping the Future of Infrastructure.pdfCheryl Hung
Keynote at DIGIT West Expo, Glasgow on 29 May 2024.
Cheryl Hung, ochery.com
Sr Director, Infrastructure Ecosystem, Arm.
The key trends across hardware, cloud and open-source; exploring how these areas are likely to mature and develop over the short and long-term, and then considering how organisations can position themselves to adapt and thrive.
The Art of the Pitch: WordPress Relationships and SalesLaura Byrne
Clients don’t know what they don’t know. What web solutions are right for them? How does WordPress come into the picture? How do you make sure you understand scope and timeline? What do you do if sometime changes?
All these questions and more will be explored as we talk about matching clients’ needs with what your agency offers without pulling teeth or pulling your hair out. Practical tips, and strategies for successful relationship building that leads to closing the deal.
23. The Immune System - includes all parts of
the body that help in the recognition and
destruction of foreign materials. White
blood cells, phagocytes and lymphocytes,
bone marrow, lymph nodes, tonsils,
thymus, and your spleen are all part of the
immune system.
24.
25. • First-Line Defenses /Innate Immune System-
The body's first line of defense against
pathogens uses mostly physical and chemical
barriers such as
• Skin – acts as a barrier to invasion
• Sweat – has chemicals which can kill different
pathogens.
• Tears - have lysozyme which has powerful
digestive abilities that render antigens harmless.
• Saliva – also has lysozyme.
• Mucus - can trap pathogens, which are then
sneezed, coughed, washed away, or destroyed
by chemicals.
• Stomach Acid – destroys pathogens
26.
27. • Second-Line Defenses - If a pathogen is
able to get past the body's first line of
defense, and an infection starts, the body
can rely on it's second line of defense. This
will result in what is called an……….
28. • Inflammatory response causes
• Redness - due to capillary dilation
resulting in increased blood flow
• Heat - due to capillary dilation resulting in
increased blood flow
• Swelling – due to passage of plasma from
the blood stream into the damaged tissue
• Pain – due mainly to tissue destruction
and, to a lesser extent, swelling.
29.
30. • Third-Line Defenses - Sometimes the second line
of defense is still not enough and the pathogen is
then heading for the body's last line of defense, the
immune system.
• The immune system recognizes, attacks, destroys,
and remembers each pathogen that enters the
body. It does this by making specialized cells
and antibodies that render the pathogens harmless.
• Unlike the first line and second line defense the
immune system differentiates among pathogens.
• For each type of pathogen, the immune system
produces cells that are specific for that particular
pathogen.
31. • An antibody is a protein produced in
response to an antigen.
• Antigens are macromolecules that elicit an
immune response in the body. The most
common antigens are proteins and
polysaccharides.
32. • Antigens can enter the body from the environment.
These include
• inhaled macromolecules (e.g., proteins on cat hairs
that can trigger an attack of asthma in susceptible
people)
• ingested macromolecules (e.g., shellfish proteins that
trigger an allergic response in susceptible people)
• molecules that are introduced beneath the skin (e.g.,
on a splinter or in an injected vaccine)
33. • antigens can be generated within the cells
of the body. These include
• proteins encoded by the genes of viruses
that have infected a cell
• aberrant proteins that are encoded by
mutant genes; such as mutated genes in
cancer cells
34. • Lymph is a milky body fluid that contains
a type of white blood cells, called
lymphocytes, along with proteins and fats.
• Lymph seeps outside the blood vessels in
spaces of body tissues and is stored in the
lymphatic system to flow back into the
bloodstream.
35. • Through the flow of blood in and out of
arteries, and into the veins, and through the
lymph nodes and into the lymph, the body is
able to eliminate the products of cellular
breakdown and bacterial invasion.
36. • There are more than 100 tiny, oval
structures called lymph nodes. These are
mainly in the neck, groin and armpits, but
are scattered all along the lymph vessels.
• They act as barriers to infection by filtering
out and destroying toxins and germs. The
largest body of lymphoid tissue in the
human body is the spleen.
37.
38. • As the lymph flows through lymph vessels,
it passes through lymph nodes.
• White blood cells called macrophages
trap and engulf cell debris and pathogens.
Other white blood cells, called
• Lymphocytes - are a type of white blood
cell capable of producing a
specific immune response to unique
antigens. They produce antibodies which
are chemicals that mark pathogens for
destruction.
39. The scanning electron micrograph above, shows a human
macrophage (gray) approaching a chain of Streptococcus
pyogenes (yellow). Riding atop the macrophage is a spherical
lymphocyte. Both macrophages and lymphocytes can be
found near an infection, and the interaction between these
cells is important in eliminating infection.
40. • Once a white cell has left the blood vessel and
migrated to the enemy, the next job is to EAT the
microbe.
• The macrophage is a large phagocyte. A
phagocyte is an eating cell (phago = "eating",
cyte = "cell") which engulfs invaders.
41. • Immunity is the result of the action of two types lymphocytes,
the B lymphocytes and the T lymphocytes.
• B cells produce antibodies that are secreted into the blood
and lymph.
• T cells attack the cells that have antigens that they
recognize.
42. Killer T Cells (lymphocytes) recognize surface
markers on other cells labeled for destruction. They,
Killer T Cells, help to keep virus-infected or malignant
cells in check.
Here, a smaller Killer T Cell (arrow) is attacking and
killing a much larger flu virus-infected target. The
sequence represents 30 minutes elapsed time.
43. • It has been estimated that during our lifetime, we
will encounter a million foreign antigens capable of
causing disease, and our bodies need the same
amount of lymphocytes to defend against them.
• There will always be a different type of lymphocyte
for each possible antigen.
44. •Active Immunity occurs when when
one makes his/her own antibodies. This
type of immunity is long term.
•Getting the disease : If you get an
infectious disease (like Chicken
Pox), often times, that stimulates the
production of MEMORY cells which
are then stored to prevent the
infection in the future.
45. Vaccination: A vaccination is an injection
of a weakened form of the actual antigen
that causes the disease. The injection is
too weak to make you sick, but your B
lymphocytes will recognize the antigen
and react as if it were the "real thing".
Thus, you produce MEMORY cells for
long term immunity.
46. Passive Immunity occurs when the
antibodies come from some other source.
This type of immunity is short term.
Breastmilk : Milk
from a mother's
breast contains
antibodies. The
baby is acquiring
passive
immunity. These
antibodies will
only last several
weeks.
47. Gamma Globulin: A Gamma Globulin shot is
purely an injection of antibodies to provide
temporary immunity. You might receive an
Gamma Globulin shot if you travel outside
of the country.
48. Types of Acquired Immunity
I. Naturally Acquired Immunity: Obtained in the
course of daily life.
A. Naturally Acquired Active Immunity:
– Antigens or pathogens enter body naturally.
– Body generates an immune response to antigens.
– Immunity may be lifelong (chickenpox or mumps) or
temporary (influenza or intestinal infections).
B. Naturally Acquired Passive Immunity:
– Antibodies pass from mother to fetus via placenta or
breast feeding (colostrum).
– No immune response to antigens.
– Immunity is usually short-lived (weeks to months).
– Protection until child’s immune system develops.
49. Types of Acquired Immunity (Continued)
II. Artificially Acquired Immunity: Obtained by
receiving a vaccine or immune serum.
1. Artificially Acquired Active Immunity:
– Antigens are introduced in vaccines (immunization).
– Body generates an immune response to antigens.
– Immunity can be lifelong (oral polio vaccine) or
temporary (tetanus toxoid).
2. Artificially Acquired Passive Immunity:
– Preformed antibodies (antiserum) are introduced
into body by injection.
• Snake antivenom injection from horses or rabbits.
– Immunity is short lived (half life three weeks).
– Host immune system does not respond to antigens.
50. Duality of Immune System
I. Humoral (Antibody-Mediated)
Immunity
– Involves production of antibodies against foreign
antigens.
– Antibodies are produced by a subset of
lymphocytes called B cells.
– B cells that are stimulated will actively secrete
antibodies and are called plasma cells.
– Antibodies are found in extracellular fluids
(blood plasma, lymph, mucus, etc.) and the
surface of B cells.
– Defense against bacteria, bacterial toxins, and
viruses that circulate freely in body fluids, before
they enter cells.
53. Duality of Immune System (Continued)
II. Cell Mediated Immunity
– Involves specialized set of lymphocytes called T
cells that recognize foreign antigens on the
surface of cells, organisms, or tissues:
• Helper T cells
• Cytotoxic T cells
– T cells regulate proliferation and activity of other
cells of the immune system: B cells,
macrophages, neutrophils, etc.
– Defense against:
• Bacteria and viruses that are inside host cells and are
inaccessible to antibodies.
• Fungi, protozoa, and helminths
• Cancer cells
• Transplanted tissue
55. Antigens
x Most are proteins or large polysaccharides
from a foreign organism.
– Microbes: Capsules, cell walls, toxins, viral
capsids, flagella, etc.
– Nonmicrobes: Pollen, egg white , red blood cell
surface molecules, serum proteins, and surface
molecules from transplanted tissue.
x Lipids and nucleic acids are only antigenic
when combined with proteins or
polysaccharides.
x Molecular weight of 10,000 or higher.
– Hapten: Small foreign molecule that is not antigenic.
Must be coupled to a carrier molecule to be antigenic.
Once antibodies are formed they will recognize hapten.
56. Antigens
Epitope:
x Small part of an antigen that interacts
with an antibody.
x Any given antigen may have several
epitopes.
x Each epitope is recognized by a
different antibody.
58. Antibodies
x Proteins that recognize and bind to a
particular antigen with very high
specificity.
x Made in response to exposure to the
antigen.
x One virus or microbe may have several
antigenic determinant sites, to which
different antibodies may bind.
x Each antibody has at least two identical
sites that bind antigen: Antigen binding
sites.
x Valence of an antibody: Number of antigen
59. Antibody Structure
x Monomer: A flexible Y-shaped molecule
with four protein chains:
– 2 identical light chains
– 2 identical heavy chains
x Variable Regions: Two sections at the end
of Y’s arms. Contain the antigen binding
sites (Fab). Identical on the same antibody,
but vary from one antibody to another.
x Constant Regions: Stem of monomer and
lower parts of Y arms.
x Fc region: Stem of monomer only.
Important because they can bind to
complement or cells.
61. Immunoglobulin Classes
I. IgG
x Structure: Monomer
x Percentage serum antibodies: 80%
x Location: Blood, lymph, intestine
x Half-life in serum: 23 days
x Complement Fixation: Yes
x Placental Transfer: Yes
x Known Functions: Enhances phagocytosis,
neutralizes toxins and viruses, protects fetus
and newborn.
62. Immunoglobulin Classes
II. IgM
x Structure: Pentamer
x Percentage serum antibodies: 5-10%
x Location: Blood, lymph, B cell surface
(monomer)
x Half-life in serum: 5 days
x Complement Fixation: Yes
x Placental Transfer: No
x Known Functions: First antibodies produced
during an infection. Effective against
microbes and agglutinating antigens.
63. Immunoglobulin Classes
III. IgA
x Structure: Dimer
x Percentage serum antibodies: 10-15%
x Location: Secretions (tears, saliva, intestine,
milk), blood and lymph.
x Half-life in serum: 6 days
x Complement Fixation: No
x Placental Transfer: No
x Known Functions: Localized protection of
mucosal surfaces. Provides immunity to
infant digestive tract.
64. Immunoglobulin Classes
IV. IgD
x Structure: Monomer
x Percentage serum antibodies: 0.2%
x Location: B-cell surface, blood, and lymph
x Half-life in serum: 3 days
x Complement Fixation: No
x Placental Transfer: No
x Known Functions: In serum function is
unknown. On B cell surface, initiate immune
response.
65. Immunoglobulin Classes
V. IgE
x Structure: Monomer
x Percentage serum antibodies: 0.002%
x Location: Bound to mast cells and basophils
throughout body. Blood.
x Half-life in serum: 2 days
x Complement Fixation: No
x Placental Transfer: No
x Known Functions: Allergic reactions.
Possibly lysis of worms.
66. How Do B Cells Produce Antibodies?
– B cells develop from stem cells in the bone
marrow of adults (liver of fetuses).
– After maturation B cells migrate to lymphoid
organs (lymph node or spleen).
– Clonal Selection: When a B cell encounters
an antigen it recognizes, it is stimulated and
divides into many clones called plasma
cells, which actively secrete antibodies.
– Each B cell produces antibodies that will
recognize only one antigenic determinant.
68. Humoral Immunity (Continued)
Apoptosis
– Programmed cell death (“Falling away”).
– Human body makes 100 million lymphocytes
every day. If an equivalent number doesn’t
die, will develop leukemia.
– B cells that do not encounter stimulating
antigen will self-destruct and send signals to
phagocytes to dispose of their remains.
– Many virus infected cells will undergo
apoptosis, to help prevent spread of the
infection.
69. Humoral Immunity (Continued)
Clonal Selection
– Clonal Selection: B cells (and T cells) that
encounter stimulating antigen will proliferate
into a large group of cells.
– Why don’t we produce antibodies against
our own antigens? We have developed
tolerance to them.
– Clonal Deletion: B and T cells that react
against self antigens appear to be destroyed
during fetal development. Process is poorly
understood.
70. Consequences of Antigen-Antibody
Binding
Antigen-Antibody Complex: Formed when an
antibody binds to an antigen it recognizes.
Affinity: A measure of binding strength.
1. Agglutination: Antibodies cause antigens
(microbes) to clump together.
• IgM (decavalent) is more effective that IgG
(bivalent).
• Hemagglutination: Agglutination of red blood
cells. Used to determine ABO blood types and to
detect influenza and measles viruses.
2. Opsonization: Antigen (microbe) is covered
with antibodies that enhances its ingestion
and lysis by phagocytic cells.
72. Humoral Immunity (Continued)
3. Neutralization: IgG inactivates viruses by
binding to their surface and neutralize toxins
by blocking their active sites.
4. Antibody-dependent cell-mediated
cytotoxicity: Used to destroy large
organisms (e.g.: worms). Target organism is
coated with antibodies and bombarded with
chemicals from nonspecific immune cells.
5. Complement Activation: Both IgG and IgM
trigger the complement system which
results in cell lysis and inflammation.
74. Immunological Memory
Antibody Titer: The amount of antibody in the
serum.
Pattern of Antibody Levels During Infection
Primary Response:
– After initial exposure to antigen, no
antibodies are found in serum for several
days.
– A gradual increase in titer, first of IgM and
then of IgG is observed.
– Most B cells become plasma cells, but some
B cells become long living memory cells.
– Gradual decline of antibodies follows.
75. Immunological Memory (Continued)
Secondary Response:
– Subsequent exposure to the same antigen
displays a faster and more intense antibody
response.
– Increased antibody response is due to the
existence of memory cells, which rapidly
produce plasma cells upon antigen
stimulation.
77. T Cells and Cell Mediated Immunity
Antigens that stimulate this response are
mainly intracellular.
Requires constant presence of antigen to
remain effective.
Unlike humoral immunity, cell mediated
immunity is not transferred to the fetus.
Cytokines: Chemical messengers of immune
cells.
– Over 100 have been identified.
– Stimulate and/or regulate immune
responses.
• Interleukins: Communication between WBCs.
78. T Cells and Cell Mediated Immunity
Cellular Components of Immunity:
– T cells are key cellular component of
immunity.
– T cells have an antigen receptor that
recognizes and reacts to a specific antigen
(T cell receptor).
– T cell receptor only recognize antigens
combined with major histocompatability
(MHC) proteins on the surface of cells.
• MHC Class I: Found on all cells.
• MHC Class II: Found on phagocytes.
– Clonal selection increases number of T
cells.
79. T Cells Only Recognize Antigen
Associated with MHC Molecules on
Cell Surfaces
80. T Cells and Cell Mediated Immunity
Types of T cells
1. T Helper (TH) Cells: Central role in immune
response.
• Most are CD4+
• Recognize antigen on the surface of antigen
presenting cells (e.g.: macrophage).
• Activate macrophages
• Induce formation of cytotoxic T cells
• Stimulate B cells to produce antibodies.
82. Types of T cells (Continued)
2. Cytotoxic T (Tc) Cells: Destroy target cells.
• Most are CD4 negative (CD4 -).
• Recognize antigens on the surface of all cells:
– Kill host cells that are infected with viruses or bacteria.
– Recognize and kill cancer cells.
– Recognize and destroy transplanted tissue.
• Release protein called perforin which forms a
pore in target cell, causing lysis of infected cells.
• Undergo apoptosis when stimulating antigen is
gone.
84. Types of T cells (Continued)
3. Delayed Hypersensitivity T (TD) Cells:
Mostly T helper and a few cytotoxic T cells
that are involved in some allergic reactions
(poison ivy) and rejection of transplanted
tissue.
4. T Suppressor (Ts) Cells: May shut down
immune response.
85. Nonspecific Cellular
Components
1. Activated Macrophages: Stimulated
phagocytes.
• Stimulated by ingestion of antigen
• Larger and more effective phagocytes.
• Enhanced ability to eliminate intracellular
bacteria, virus-infected and cancerous cells.
2. Natural Killer (NK) Cells:
• Lymphocytes that destroy virus infected and
tumor cells.
• Not specific. Don’t require antigen stimulation.
• Not phagocytic, but must contact cell in order to
lyse it.
86. Relationship Between Cell-Mediated and
Humoral Immunity
1. Antibody Production
T-Dependent Antigens:
– Antibody production requires assistance from T helper
cells.
– A macrophage cells ingest antigen and presents it to TH cell.
– TH cell stimulates B cells specific for antigen to become
plasma cells.
– Antigens are mainly proteins on viruses, bacteria, foreign
red blood cells, and hapten-carrier molecules.
T-Independent Antigens:
89. Relationship Between Cell-Mediated and
Humoral Immunity
2. Antibody Dependent Cell Mediated
Cytotoxicity
– Target cell is covered with antibodies, leaving Fc
portion sticking outwards.
– Natural killer and other nonspecific cells that have
receptors for Fc region are stimulated to kill
targeted cells.
– Target organism is lysed by substances secreted
by attacking cells.
–