neoplasia
new growth
=> tumor
neoplastic cells are
transforemd
-> dont respond to inhibitory growth signals
-> a degree of autonomy
-> need host for nutrition and blood supply
Benign
its microscopic and gross characteristics are considered to be relatively innocent, implying that it will remain localized and is amenable to local surgical remova
Malignant
implies that the lesion can invade and destroy adjacent structures and spread to distant sites (metastasize) to cause death
2 components of tumor
parenchyme -> part of tumor that grows (dtermines benign/malignant) neoplstic
stroma -> supply tuor with blood non neopalstic
Bening tumors
Attach the suffix – oma to cell type from which the tumor arise: easy for mesenchimal tumors
Epithelial or mesenchymal cells
Fibrous tissue – fibroma
Cartilage – chondroma chondrocytes
Bone – osteoima
More complex nomenclature is applied to benign epithelial tumor
types Malignant tumors
carcinoma
sarcoma
Carcinoma
epithelial malignant tumor
Adenocarcinoma
• Carcinomas that grow in glandular pattern, or arise from glandular epithelial cells
Squamous cell carcinoma
• Carcinomas which arise from squamous cells
Teratoma
Tumours which originate from totipotential germ cell in ovary, testis and sometimes in midline embryonic rest
Germ cells have capacity to differentiate into any ofthe cell types found inthe adult body
Mixed tumors – tumors with divergent
differentiation
Progenitor cell in this tumors has the capacity to differentiate down more than one lineage
Hamaratoma
Mass of disorganised tissue which contain the same tissue as the organ in which it is found
Choristoma
Congenital anomaly consisting of a heterotopic nest of the cell
-oma is bening EXEPT
Lymphoma
Sacroma
Melanoma
Seminoma
differentiation and anaplasia
Extent to which neoplasms resemble their cells of origin, both morphologically and functionally
Anaplasia is lack of differentiation – loss of the structural and functional differentiation of normal cells
Benign neoplasms are well differentiated, never anaplastic
Malignant neoplasms range from well differentiated to poorly differentiated and anaplastic
• ANAPLASIA= MALIGNANT!!!
Characteristics of anaplastic cells
Pleomorphism = Variation in size and shape
• Nuclear abnormalities= Hypechromatism, variation in size
and shape, prominent single or multiple nucleoli
• Increased nuclear cytoplasmatic ratio
• Tumor giant cells
• Atypical mytosis= Tripolar or quadripolar mitotic figures Loss of polarity
local invasion of bening tumor
growth slowly and develop a rim of compressed fibrous tissue
local invation of cancer
progressive infiltration , invasion, and destruction of surrounding tissue
most common targets for metastasis
liver & lung
bening dont metastasize
environmental factors
Environmental exposures appear to be the dominant risk factors for many common cancers, suggesting that a high fraction of cancers arepotentially preventable. The role of genetic factors!
-> arsen
-> asbest
-> benzene (myeloid)
predisposing factors
chronic inflammation -> carcinoas
immunodeficiency -> lymphomas
Driver mutation
is an alteration that gives a cancer cell a fundamental growth advantage for its neoplastic transformation. Most of them are acquired, but can be inherited
Passenger mutations
Passenger mutations do not directly drive cancer initiation and progression, but contribute to carcinogen-associated cancer and tumor drug resistance to therapy. Always acquired
point mutation
Protoongogenes to oncogenes = gain of function (RAS)
tumor supressor genes = loss of function (TP53)
gene rearrangements, deletions, gene amplifications
can also cause tumors
2 important examples of amplification
NMYC gene -> neuroblastoma
HER2 -> breast cancer
Hallmarks of cancer
Self-suffciency in growth signals
Insensitivity to growth-inhibitory signals
Altered cellular metabolism
Evasion of apoptosis
Immortality
Sustained angiogenesis
Invasion and metastasis
Evasion of immune survelliance
role of cyclins CDKs and CKD inhibitor
Cyclin D-CDK4, cyclin D-CDK6, and cyclin E-CDK2 regulate the G1-to-S transition by phosphorylating the Rb protein (pRb).
Cyclin A-CDK2 and cyclin A-CDK1 are active in the S phase. Cyclin B-CDK1 is essential for the G2-to-M transition.
Two families of CDK inhibitors can block activity of CDKs and progression through the cell cycle.
The so-called “INK4 inhibitors,” composed of p16, p15, p18, and p19, act on cyclin D-CDK4 and cyclin D-CDK6.
The other family of 3 inhibitors p21,p27 and p57 can inhibit all CDKs
RB (governor of the cell cycle)
• Hypophosphorylated RB + E2F= transcriptional block
Hyperphosphorylated RB = free E2F= transcriptional activation
One of the four key regulators of the cell cycle (p16, cyclinD, CDK4, RB) is mutated in most human cancers!!!
TP53 (guardian of the genome)
• TP53= central monitor of sress in the cell
• DNA damage leads to p53 activation by phosphorylation inducing CDKNIA (p21) which prevents RB phosphorylation and leads to G1-S block in the cell cycle
most commonly muted supressor gene
Becacizumab
blocks angiogenesis -> slows cancer growth
invasion and metastasis
Loosening of the intracellular junctions between tumor cells by loosing E-cadherin function
Degradation of basment membrane and interstitial connective tissue by
MMPs,cathesin D,...
Loos of adhesion to ECM proteins
Locomotion leading tumor cells through basment membrane and ECM
tumor antigens
• Neoantigenes:newly formed antigenes due to genetc mutations • Preexisting proteins expressed by tumor cells:
- Tyrosinase ; expressed only in normal melanocytes and melanomas
- Cancer-testis-antigenes; expressed only in the germ cells in the testis
• Viral proteins as antigenes
clinical features due to cancer
• Progressive loss of body fat and lean body mass
• Anemia
• Weakness
• Anorexia
=> weight loss
paraneoplastic syndrome
occures in patients with cancer but cant be explained with it
hypercalemia
chushing syndrome
nonbacterial thrombotic endocarditis
what is the most commony mutated oncogene?
RAS
BRAF (in melanomas)
Adenoma
eip. tumors arrising di glands or forming glandular patterns
cystadenoma
adenomaaas producing larde cystic masses common in ovary
papillomas
epithelial tumors forming gross or microscopic fingerlike projections
polyp
tumor projecting macroscopically above the mucosa (colon polyp)
Last changed9 months ago