L3.Neoplasia _Genetics.pdf

Transcript

pathophysiology
PATH200 & 310/MACHS

Lecture-3 :Neoplasia & Genetics

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 Outlines
Adaptive changes and causes of cellular adaption.
Genetic control of cell function and inheritance.
Mechanisms of inheritance
Genetic and congenital disorders
Neoplasm – terminology
Differentiating between benign and malignant tumors.
Cancer and carcinogenesis process
Pathophysiology of the malignant process
Tumor staging and grading
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 LEARNING
OBJECTIVES

By the end of this lecture each
student will be able to :
◼ Describe the Cell injury and
Cellular Adaptive Changes.
◼ Discuss the common congenital
disorders
◼ Explain the definition of
neoplasia
◼ Differentiate between benign
tumor and malignant tumor
◼ Describe the TNM system.
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 INTRODUCTION

◼ The life cycle of a cell exists on continuum that includes normal
activities and adaptation, injury or lethal changes.

◼ Adaptive changes- Prevention of disease by the body depends on
the capacity of the affected cells to undergo self-repair and
regeneration
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 CAUSES OF CELLULAR ADAPTION

When cells are confronted to one of the following stimulus, they may undergo adaptive changes
a) Physical agents - Trauma, Burn, pressure, irradiation, etc
b) Chemical agents - Poisons, drugs, simple compounds, etc.
c) Micro organisms – Bacteria, Virus, Fungus, Parasites
d) Hypoxia - most common cause. Is because of inadequate oxygen in the blood or decreased tissue
perfusion.
e) Genetic defects - Can affect cellular metabolism through inborn errors of metabolism or gross
malformation
f) Nutritional imbalances
g) Immunologic reaction E.g. - Hypersensitivity reaction.
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Refers to prevention of disease by the body depends on the capacity of the
affected cells to undergo self-repair and regeneration.

a. Physiological changes

b. Biological changes

c. Adaptive changes

d. Chemical changes

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Which of the following adaptive changes occurs due to inadequate oxygen in
the blood or decreased tissue perfusion?

a. Physical agents

b. Chemical agents

c. Micro organisms

d. Hypoxia

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 TYPES OF CELLULAR ADAPTIVE-CHANGES
When cells are exposed to one of the above noxious stimulus, they will undergo one or more

of the following types of adaptive changes:-

I. Abnormal accumulation of intracellular substances

II. Changes to cellular size or numbers

III. Cellular injury and lethal changes

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 I. Abnormal Accumulation Of Intracellular Substances

Due to environmental changes or an inability of the cell to process materials
(substances) that cannot be metabolized by the cells, these substances may accumulate
in the cytoplasm. As a result, common changes include:-
◼ Cellular swelling
◼ Lipid accumulation
◼ Glycogen depositions.
◼ Calcification
◼ Hyaline infiltration

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II.Changes To Cellular Size Or Numbers

Result of response to adaptation to harmful agents
I) Atrophy: refers to a decrease in cell size.
II) Dysplasia:- Dysplasia refers to the appearance of cells that have undergone some atypical
changes in response to chronic irritation.
III) Hyperplasia: increase of tissue mass due to an increase in the number of cells.
IV) Hypertrophy: increase in the size of individual cells, resulting in increased tissue mass with
out an increase in the number of cells.
V) Metaplasia: one type of adult cell is replaced by another type.

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Refers to the appearance of cells that have undergone some
atypical changes in response to chronic irritation

a. Atrophy
b. Dysplasia
c. Hyperplasia
d. Hypertrophy

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III. Cellular Injury And Lethal Changes
Cell injury can be sub lethal or lethal.
Sub lethal injury alters functions with out causing cell death. The changes caused by this
type of injury are potentially reversible if the injuring stimuli are removed.
Causes of Cell Injury
◼ Hypoxia and ischemia
◼ Toxins
◼ Infectious agents
◼ Immunologic reactions
◼ Nutritional imbalances
◼ Genetic abnormalities
◼ Physical agents
◼ Aging
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TYPES OF CELLULAR INJURY

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REVERSIBLE CELL INJURY
◼ Cell injury which can be reversed when the
stimulus or the cause of injury is removed.

Causes
◼ Ischemia: critical lack of blood supply to
a localized area.

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 Irreversible Cell Injury
◼ It is cellular injury that can not be corrected (reversed) after the
stimulus or cause has been removed.
a. Infarction:- Is localized area of tissue death due to lack of blood
supply. It is due to occlusion of blood vessels by thrombus or embolus.
b. Necrosis: cell or tissue death characterized by structural evidence of
this death.
c. Apoptosis : programmed cell death or “clean” form of cell suicide
occurring in pathologic situations
When a cell's DNA or proteins are damaged beyond repair or cells destined to
die activate their own enzymes to degrade their own nuclear DNA and
proteins

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Genetic Control Of Cell Function And Inheritance

Nucleus contains the chromosomes
Chromosomes: Discrete bundles of DNA containing genetic information, Arranged in
pairs; one from the mother and one from the father
Humans have 23 pairs of chromosomes,22 are autosomes , 23rd pair are the sex chromosomes
(determine the sex of an individual)

DNA -Long, double-stranded helical structure composed of nucleotides, which consist of phosphoric acid,
deoxyribose, and one of four nitrogenous bases (Thymine (T),Cytosine (C),Adenine (A),Guanine (G))

Gene -a part of the DNA molecule that contains the information needed to code for the types of
proteins and enzymes needed for the day-to-day function of the cells in the body.
A gene is the unit of heredity passed from generation to generation

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 Mechanisms Of Inheritance: Cell Division

◼ Cells form two groups based on function:
◼ Body (somatic)cells: form the structures of the
body
◼ Reproduce by mitosis: Forming two identical
cells, each equipped with 23 pairs of
chromosomes
◼ Germ cells: form the reproductive cells
◼ Reproduce by meiosis: forming four cells with
each cell containing only 23 chromosomes
◼ These cells are the gametes: ova or sperm
◼ During conception, a sperm merges with an
ovum to form a new cell containing 23 pairs of
PATH200/MACHS
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 GENETIC DISORDERS

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 Genetic and Congenital Disorders

Congenital conditions are those present from birth. Birth defects are described as
being congenital. They can be caused by
◼ Genetic Factors -chromosomal aberrations
◼ Environmental Factors (Fetal Development)-Maternal disease, infections, or
drugs taken during pregnancy
◼ Intrauterine Factors (Rare)-Fetal crowding, positioning

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 Genetic and Chromosomal Disorders
◼ Genetic disorders represent changes (or mutations) in gene function or changes in
chromosomal structure.
◼ The effects of an abnormal genetic trait may present at birth or may not
become apparent until later in life.
1. Single gene Disorders -Caused by a single defective or mutant gene
2. Disorders of Autosomal Inheritance -Autosomal Dominant Eg: Marfan
Syndrome, Autosomal Recessive Eg: Sickle cell disease
The key difference between autosomal dominant and autosomal recessive disorders is
that, in autosomal dominant disorders, one altered copy of a gene is enough to cause
the disease while, in autosomal recessive disorders, both altered copies of the gene are
needed to cause the disease.
3. Disorders of Sex- Linked Inheritance - Always associated with the X chromosome
4. Chromosome disorders 22
Autosomal Dominant Disorders
Marfan Syndrome:
A connective tissue disorder manifested by changes
in the skeleton, eyes, and cardiovascular system
◼ Tall and slender build.

◼ Disproportionately long arms, legs and fingers.

◼ A breastbone that protrudes outward or dips inward.

◼ A high, arched palate and crowded teeth.

◼ Heart murmurs.

◼ Extreme nearsightedness.

◼ An abnormally curved spine.

◼ Flat feet 23
Autosomal dominant disorders

◼ Neurofibromatosis (NF)
A condition involving neurogenic tumors
that arise from Schwann cells and other
elements of the peripheral nervous system
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 Autosomal recessive disorders
◼ Phenylketonuria (PKU)
◼ A rare metabolic disorder caused by a deficiency of the liver enzyme
phenylalanine hydroxylase.
◼ PKU is caused by a defect in the gene that helps create the enzyme needed to break
down phenylalanine.

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 X-linked Disorder
Hemophilia A
Disorder where the blood cannot clot properly due to a deficiency of a clotting
factor called Factor VIII. This results in abnormally heavy bleeding that will not stop,
even from a small cut

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 Chromosome Disorders
Chromosome disorders involve a change in
chromosome number or structure that results in
damage to sensitive genetic mechanism or in
reproductive disorders.
◼ Monosomy X (Turner’s syndrome)
◼ Poly somy X (Klinefelter’s syndrome)

◼ Trisiomy 21 (Down’s syndrome) - Presence of all
or part of a third copy of chromosome 21,
associated with physical growth delays, mild to
moderate intellectual disability, and characteristic
facial features
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 NEOPLASIA

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 NEOPLASM - TERMINOLOGY
◼ Neoplasm: - New abnormal growth because of abnormal cellular-
reproduction. It is synonymously used with tumor.
◼ Tumor: - A growth of Neoplastic cells clustered together to form a mass. It can
be benign or malignant.
◼ Benign tumor: - Is characterized by abnormal cell division but no metastasis or
invasion of the surrounding tissues.
◼ Malignant tumor: - Abnormal cell division characterized by ability to invade
locally, metastasize and reoccur. It is cancer cells.
◼ Carcinogenesis: - production or origination of cancer cells.
◼ Metastasis: - Ability to establish secondary tumor growth at a new location
away from the primary tumor.
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 Factors Differentiating Benign and Malignant Tumors
Benign
Malignant
◼ Similar to cell of origin
◼ Dissimilar from cell of origin
◼ Edges move out word smoothly
◼ Edges move outward irregularly.
◼ Compress locally
◼ Invade locally
◼ Slow growth rate
◼ Rapid to very rapid growth rate.
◼ Seldom Recur after removal by surgery
◼ Frequently recur after removal
◼ Necrosis and ulceration is uncommon
◼ Necrosis and ulceration common.
◼ Systemic effect is uncommon
◼ Systemic effect is common
◼ No metastasis
◼ Metastasis is common

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https://www.youtube.com/watch?v=ZcVSHYl_THE
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 CANCER
◼ Disease process that begins when a cell is transformed by genetic mutation of
cellular DNA
◼ Growth is uncoordinated and relatively autonomous.
◼ Lacks normal regulatory controls over cell growth and division
◼ Tends to increase in size and grow after stimulus ceases or needs of the organism are met

Causes: Heredity, Hormones, Immunologic mechanisms, carcinogens like Chemicals,
Radiation, Oncogenic viruses

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 CARCINOGENESIS
Malignant transformation, or carcinogenesis, is thought to be at least a three-step
cellular process:
◼ Initiation : Initiators (carcinogens), such as chemicals, physical factors, and
biologic agents, alter the genetic structure of the cellular DNA.
◼ Promotion: Repeated exposure to promoting agents (co-carcinogens) causes the
expression of abnormal or mutant genetic information
◼ Progression: The cellular changes formed during initiation and promotion now
exhibit increased malignant behavior. These cells now show a propensity to
invade adjacent tissues and to metastasize..

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 Pathophysiology of The Malignant Process

◼ Cancer is a disease process that begins when an abnormal cell is transformed
by the genetic mutation of the cellular DNA.
◼ This abnormal cell begins to proliferate abnormally
◼ The cells acquire invasive characteristics, and changes occur in surrounding
tissues.
◼ The cells infiltrate these tissues and gain access to lymph and blood vessels,
which carry the cells to other areas of the body.This phenomenon is called
metastasis (cancer spread to other parts of the body).

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Methods By Which Cancer Spreads

◼ Direct invasion and extension

◼ Seeding of cancer cells in body cavities

◼ Metastatic spread through the blood or
lymph pathways

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 Tumor Staging And Grading
◼ Staging determines the size of the tumor and the existence of metastasis. The TNM
system is frequently used.
◼ T -the extent of the primary tumor
◼ N -lymph node involvement
◼ M -the extent of metastasis

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 TNM Classification System
T The extent of primary tumor
N The absence or presence and extent of regional lymphnode metastasis
M The absence or presence of distant metastasis
Primary Tumor(T)
Tx Primary tumor cannot be assessed
T0 No evidence of primary tumor
Tis Carcinoma in situ
T1,T2,T3,T4 Increasing size and/ or local extent of the primary tumor
Regional Lymph Nodes(N)
Nx Regional lymphnodes cannot be assessed
N0 No regional lymph node metastasis
N1,N2,N3 Increasing involvement of regional lymph nodes
Distant Metastasis (M)
Mx Distant metastasis cannot be assessed
M0 No distant metastasis
M1 Distant metastasis 39
Clinical Manifestations of Cancer
◼ Tissue Integrity -Compressed and eroded blood vessels; ulceration and necrosis; frank
bleeding and hemorrhage
◼ Cancer Cachexia -Weightloss and wasting of body fat and muscle tissue; profound
weakness, anorexia, and anemia
◼ Paraneoplastic Syndromes -Inappropriate
hormone release, circulating hematopoietic,
neurological, and dermatological factors
Diagnostic Measures for Cancer Detection
Screening for early detection
Lab tests, Biopsy, Endoscopic examinations, Ultrasound, X-ray studies, MRI, CT and PET ,Tumor markers

Treatment
Surgery, Chemotherapy, radiotherapy, Hormone therapy , Immunotherapy, Palliative treatment 40
 REFERENCES
 NORRIS, T. (2019). Porth’s Pathophysiology Concepts of Altered
Health States. 10th ed. Wolters Kluwer
 Ian Peate, (2021) Fundamentals of applied pathophysiology: an
essential guide for nursing & healthcare students. 4th ed.
 Hoboken, NJ : Wiley-Blackwell Dignle, M., Mulvihill, M., Zelman,
M. & Tompary, E. (2011). Introductory pathophysiology for nursing
& healthcare professionals. |Pearson
 Nair, M., & Peate, I. (2015). Pathophysiology for nurses at a glance
(nursing and healthcare). Publisher: West Sussex, England: John Wiley
& Sons, Inc

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