Pathology Neoplasia Lec. 1 PDF

Summary

This document provides an overview of pathology, focusing on neoplasia. It describes the definition, characteristics, and classification of different types of tumors, including benign and malignant tumors. It also covers the incidence and significance of neoplasms. The document is suitable for medical students and professionals.

Full Transcript

Lectures No. 1
PATHOLOGY Dr. Nazar Jewher

Neoplasia - 1
Definition:
Literally:
▪ It is an abnormal mass of tissue the growth of which exceeds & is
uncoordinated with that of the normal tissues & persists in the same
excessive manner after cessation of the stimuli that evoked the
change.
▪ It is purposeless, preys on the host & is autonomous (loss of
responsiveness to normal growth control).
▪ It behaves like a parasite, competes with normal tissue for their
metabolic needs.
▪ Cancer is not one disease but many disorders that share a profound
growth dysregulation.
▪ Results from genetic alterations that are passed down to the
progeny of the tumor cells. These genetic changes allow excessive
and unregulated proliferation that becomes autonomous
(independent of physiologic growth stimuli),

Oncology:
▪ Tumor: Swelling.

▪ Cancer: A common term for all type of malignant tumors. Derived
from the Latin cancer (for crab), because cancer adheres to any
part that seizes upon in an obstinate manner like a crab.

INCIDENCE:
▪ More than 1 million individuals develop cancer every year, and cancer
causes more than 560000 annual deaths in the state.

▪ It is the second leading cause of death after cardiovascular diseases.

▪ Neoplasms are important not only because of the mortality rate but
also because of the great physical and emotional impact they inflict
on the patients and their families.
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▪ Recently, there has been dramatic improvements in the survival
rates in some cancers ( especially leukemias & lymphomas). A
greater proportion of cancers are being cured or arrested today than
ever before.

▪ The only hope for controlling cancer lies in learning more about its
etiology & pathogenesis.

Classification:

Clinically Tumors Are Classified Into:
1. Benign tumors:
2. Malignant tumors:
3. Borderline malignant tumors:

1. Benign tumors: Characterized by
▪ Innocent features.
▪ Localized.
▪ Cannot spread.
▪ Surgical excision.
▪ No affect survival.

2. Malignant tumors:
▪ Morphological features.
▪ Invade & destroy.
▪ Metastasize).
▪ Can cause death.

3. Borderline malignant tumors:

Nomenclature
All tumors have two basic components:
▪ Proliferating neoplastic cells that constitute the parenchyma.
▪ Supportive stroma made up of connective tissue & blood vessels

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NOTE:
Some tumors have scanty stroma so the neoplasm is soft & fleshy,
other tumors especially some cancers stimulate the formation of an
abundant collagenous stroma ( referred to as desmoplasia) imparting a
stony hard consistency to the tumor ( as scirrhous carcinoma of the
breast).
▪ Tumor either arises from epithelial cells, mesenchymal cells,
hemopoietic, lymphoid cells, nerve cells, or from totipotential cells.

▪ Any of these tumors could be benign or malignant.

▪ Tumors are named according to the type of cells from which they
arise or according to the tissue they resemble.

BENIGN TUMORS
Are designated by attaching the suffix –Oma to the cell of origin. Either of
benign epithelial tumors or benign mesenchymal tumors:

Benign Epithelial Tumors:
⚫ Adenoma:
Applied to benign tumor derived from glands (e.g. salivary, sweat
glands) or tumor forming glandular pattern (renal cell adenoma).

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⚫ Papilloma:
Benign epithelial neoplasm that
produces finger like projections
from epithelial surfaces (e.g.
squamous papilloma).

⚫ Cystadenoma:
Benign tumor producing hollow cystic mass,
mostly seen in the ovary. Sometimes papillary
cystadenoma.

⚫ Polyp:
Benign epithelial tumor produces a mass that projects above a mucosal
surface. Mostly seen in the GIT.

Benign Mesenchymal Tumors
▪ Named by attaching the suffix –Oma to the cell of origin.
▪ Example: fibroma. Lipoma, neuroma, leiomyoma, osteoma,
chondroma….

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MALIGNANT TUMORS

Carcinoma:
Malignant tumors of epithelial cell origin. They are further classified into:
▪ Squamous cell carcinoma.
▪ Adenocarcinoma.
▪ Transitional cell carcinoma.
▪ Basal cell carcinoma.

Sarcoma:
Malignant tumors arising from mesenchymal tissues.e.g.,
▪ Fibrosarcoma
▪ Liposarcoma
▪ Leiomyosarcoma
▪ Osteosarcoma ,Etc.

MIXED TUMORS
▪ This term applied to a small group of tumors that are composed of
a mixture of epithelial & mesenchymal components. They result
from divergent differentiation of a single line of parenchymal cells.

▪ Benign mixed tumors: e.g., pleomorphic adenoma ( These tumors
contain epithelial components scattered within a myxoid stroma
that sometimes contains islands of cartilage or bone),
fibroadenoma,

▪ Malignant mixed tumors: e.g., malignant mixed tumor of the salivary
gland & carcinosarcoma.

TERATOMA
▪ This tumor arises from totipotential cells, so they have the capacity
to differentiate into any cell types present in the body i.e., it
contains tissue representative of more than one germ layer.

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▪ Since they arise from totipotential cells, so they are principally
encountered in the gonads (although rarely found in sequestered
rest). e.g. dermoid cyst of the ovary. Teratoma could be benign or
malignant.

N.B: There are some exception to this nomenclature e.g. lymphoma,
melanoma, glioma, seminoma , ……..

Table: Nomenclature of tumors

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⚫ What Is Hamartoma?
▪ aberrant differentiation produce mass or developmental
malformation

1. consist of mature tissues but disorganized
2. tissues related to site of origin.

▪ e.g. lung hamartoma: islands of cartilage/blood vessels/bronchial
mucosa

⚫ What Is Choristoma?

▪ presence of a normal tissue in an unexpected location e.g.
pancreatic tissue in wall of esophagus or stomach or small
intestine, may form masse mimicking neoplasm grossly.

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CHARACTERISTIC OF BENIGN & MALIGNANT TUMORS
⚫ The differentiation between benign and malignant tumors is one of
the most important distinctions a pathologist can make. In the great
majority of instances, a benign tumor may be distinguished from a
malignant tumor with considerable confidence on the basis of:

▪ Differentiation & anaplasia:
▪ Rate of growth:
▪ Local invasion:
▪ Metastasis:

Differentiation & Anaplasia
⚫ Refers to the extent to which parenchymal neoplastic cells resemble
comparable normal cells, both morphologically & functionally.

⚫ Neoplasm could be:
✓ Well-differentiated
✓ Moderately differentiated
✓ Poorly differentiated
✓ Undifferentiated

⚫ Benign tumors are well differentiated. Malignant tumors vary from
well- undifferentiated.

⚫ Anaplasia implies a reversal of differentiation to a more primitive
level. It usually results from lack of differentiation rather than
dedifferentiation.

⚫ Determination of differentiation depends on a no. of morphological
changes:

✓ Architectural pattern &Cytological features (degree of atypia):

✓ No. of mitosis &configuration:.
✓ Others as loss of polarity, tumor giant cells, necrosis

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Adenomatous polyp of the colon. Well differentiated tumor. The glands
are well-formed and normal-looking

Malignant tumor (adenocarcinoma) of the colon. The cancerous glands are
irregular in shape and size and do not resemble the normal colonic
glands. This tumor is considered differentiated because gland formation
can be seen. The malignant glands have invaded the muscular layer of the
colon.

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The normal squamous epithelium at the left merges into the squamous
cell carcinoma at the right, which is infiltrating downward. The neoplastic
squamous cells are still similar to the normal squamous cells, but are
less orderly. This is a well-differentiated squamous cell carcinoma

Here is a moderately differentiated squamous cell carcinoma in which
some, but not all, of the neoplastic cells in nests have pink keratin. In
general, neoplasms with less differentiation are more aggressive.

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The microscopic appearance of a leiomyoma indicates that the cells do
not vary greatly in size and shape and closely resemble normal smooth
muscle cells.

Lipoma: Mature fatty tissue

The microscopic
appearance of the pituitary
adenoma is shown here.
Note the monotonous
appearance of these small
round cells,
i.e no pleomorphism. This
is a well differentiated
tumor.

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This neoplasm is so poorly differentiated that it is difficult to tell what the
cell of origin is. It is probably a carcinoma because of the polygonal
nature of the cells. Note that nucleoli are numerous and large in this
neoplasm. Neoplasms with no differentiation are said to be anaplastic.

Anaplastic tumor of the skeletal muscle (rhabdomyosarcoma). Note the
marked cellular and nuclear pleomorphism, hyperchromatic nuclei, and
tumor giant cells.

Mitotic figure is seen in
the center

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Here are three abnormal mitoses. Mitoses by themselves are not indicators of
malignancy. However, abnormal mitoses are highly indicative of malignancy.
The marked pleomorphism and hyperchromatism of surrounding cells also
favors malignancy.

This sarcoma has many mitoses. A very large abnormal mitotic figure is
seen at the right.

▪ The better the differentiation of the transformed cell, the more
completely it retains the functional capabilities found in its normal
counterparts. Thus, benign neoplasms of endocrine glands
frequently elaborate the hormones characteristic of their origin.
Increased levels of these hormones in the blood are used clinically
to detect and follow such tumors. Well- differentiated squamous cell
carcinomas of the epidermis elaborate keratin, just as well-
differentiated hepatocellular carcinomas elaborate bile.
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▪ Highly anaplastic undifferentiated cells, whatever their tissue of
origin, lose their resemblance to the normal cells from which they
have arisen.

▪ Despite exceptions, the more rapidly growing and the more
anaplastic a tumor, the less likely it will have specialized functional
activity. The cells in benign tumors are almost always well
differentiated and resemble their normal cells of origin; the cells in
cancer are more or less differentiated, but some derangement of
differentiation is always present

Rate of growth
▪ In general, most benign tumors grow slowly over a period of years,
whereas most cancers grow rapidly and the rate of growth of
malignant tumors correlates with their level of differentiation. HOW?

▪ There are some exceptions to this generalization.

Local invasion
▪ Nearly all benign tumors grow as cohesive expansile masses that
remain localized to their site of origin and do not have the capacity to
infiltrate, invade, or metastasize to distant sites, as do malignant
tumor.

▪ Because they grow and expand slowly, they usually develop a rim of
compressed connective tissue, sometimes called a fibrous capsule,
which separates them from the host tissue.

▪ This capsule is derived largely from the extracellular matrix of the
native tissue due to atrophy of normal parenchymal cells under the
pressure of an expanding tumor. Such encapsulation does not
prevent tumor growth, but it keeps the benign neoplasm as a
discrete, readily palpable, and easily movable mass that can be
surgically enucleated. Some benign tumors are not encapsulated. For
example, hemangiomas (neoplasms composed of tangled blood
vessels) are often unencapsulated and may appear to permeate the
site in which they arise.
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Benign Tumor
▪ Cohesive expansile growth. Encapsulated. Localized,
circumscribed &mobile. Amenable to surgical resection
(enucleation).

▪ N.B: Not all benign tumors are encapsulated.

Uterus with leiomyomas of varying size, but all benign and well-
circumscribed firm white masses.

Malignant Tumor
▪ The growth of cancers is accompanied by progressive
infiltration, invasion, and destruction of the surrounding tissue.

▪ In general, malignant tumors are poorly demarcated from the
surrounding normal tissue, and a well- defined cleavage plane
is lacking. Most malignant tumors are obviously invasive and
can be expected to penetrate the wall of the colon or uterus, for
example, or fungate through the surface of the skin. They
recognize no normal anatomic boundaries. Such invasiveness
makes their surgical resection difficult or impossible.

▪ Progressive infiltration, invasion, & destruction of adjacent
tissues. Not encapsulated (no plane of cleavage). Excision with
safety margin.

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▪ N.B: Next to the development of metastasis, local invasion is
the most reliable feature that distinguishes malignant from
benign tumors.

Cut section of an invasive ductal carcinoma of the breast. The lesion is
retracted, infiltrating the surrounding breast substance, and would be
stony hard on palpation.

Metastasis
▪ Indicates the development of secondary implants away from the
site of primary tumor. Is the single most important feature that
distinguishes malignant from benign tumors.

▪ The probability of metastasis increases as the primary tumor
becomes more aggressive, the more rapidly growing, and the
larger the primary neoplasm, the greater the likelihood that it
will metastasize

▪ Benign tumors do not metastasis. All malignant tumors
eventually metastasis except:

▪ Approximately 30% of newly diagnosed patients with solid
tumors present with distant metastasis. Metastasis strongly
reduces the probability of cure.

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Pathways Of Spread:
A. Lymphatic Spread:
▪ is the most common pathway for the initial dissemination of
carcinomas. The pattern of lymph node involvement follows the
natural routes of lymphatic drainage.

▪ Enlargement of regional lymph nodes may be caused by:
1. The spread and growth of cancer cells or
2. Reactive hyperplasia.

▪ Therefore, nodal enlargement in proximity to a cancer, while it
must arouse suspicion, does not necessarily mean dissemination
of the primary lesion.

The Sentinel Node
To avoid the considerable surgical morbidity associated with a full
axillary lymph node dissection, biopsy of sentinel nodes is often used to
assess the presence or absence of metastatic lesions in the lymph
nodes.
A sentinel lymph node is defined as "the first node in a regional lymphatic
basin that receives lymph flow from the primary tumor.“
Sentinel node mapping can be done by injection of radiolabeled tracers
and blue dyes, and the use of frozen section upon the sentinel lymph
node at the time of surgery can guide the surgeon to the appropriate
therapy. Sentinel node biopsy has been used for detecting the spread of
melanomas, colon cancers, and other.

B. Hematogenous Spread: (Artery Vs Vein, Favored Sites)
▪ Arteries, with their thicker walls, are less readily penetrated
than are veins. With venous invasion the blood-borne cells follow
the venous flow draining the site of the neoplasm, and the tumor
cells often come to rest in the first capillary bed they encounter.

▪ Understandably the liver and lungs are most frequently involved
in such hematogenous dissemination, because all portal area
drainage flows to the liver and all caval blood flows to the lungs.

▪ Other. N.B: Carcinoma vs sarcoma
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C. Seeding The Body Cavities:
▪ Occur whenever a malignant neoplasm penetrates into a body
cavity as peritoneum & pleura. Such seeding is particularly
characteristic of carcinomas arising in the ovaries, when, not
infrequently, all peritoneal surfaces become coated with a heavy
layer of cancerous glaze.

Microscopically, metastatic adenocarcinoma is seen in a lymph node
here. It is common for carcinomas to metastasize to lymph nodes. The
first nodes involved are those draining the site of the primary.

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DYSPLASIA
▪ Disordered growth.
▪ Dysplasia is encountered principally in epithelia. It means an
abnormal but yet non-neoplastic proliferation of cells as a result
of injury. There is loss of uniformity of the individual cells and
loss of architectural orientation.
▪ Grading of dysplasia:
▪ Epithelial dysplasia does not indicate cancer but almost antedates
the appearance of cancer ( i.e premalignant). The probability of
progression depends on:

Carcinoma in situ
▪ This term indicates the presence of severe architectural and
cytological atypia in the epithelium (i.e., malignant features) BUT
such changes are confined to the epithelium & do not extend
beyond the basement membrane into the adjacent or subjacent
tissue.

▪ This is the next step toward neoplasia. Here, there is normal
cervical squamous epithelium at the left, but dysplastic squamous
epithelium at the right. Dysplasia is a disorderly growth of
epithelium, but still confined to the epithelium. Dysplasia is still
reversible.

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▪ When the entire epithelium is dysplastic and no normal epithelial
cells are left, then the process is beyond dysplasia and is now
neoplasia. If the basement membrane is still intact, as shown
here, then the process is called "carcinoma in situ" because the
carcinoma is still confined to the epithelium.

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