lecture 8: cancer as a genetic disease
TRANSCRIPT
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Cancer as a Genetic Disease
Sharon Krag, PhDJohns Hopkins University
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Section A
Introduction
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About Cancer
Cancer refers to at least 100 forms of diseaseCancer is an infectious diseaseCancer is a disease of agingCancer is an environmental disease
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About Cancer
Cancer is a genetic disease− Not monogenic like MD or CF, but multigenic
Cancer is caused by mutations in somatic cellsCancer can be caused by mutagens, chemicals that damage DNA, or virusesCancer is caused by an accumulation of mutations in different genes in a single cellCancer is caused by altered expression of genes or by accumulation of mutations in a single cell
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Mutations
Mutations, or damage to the genome, can be caused by mistakes during normal DNA replication− 1 x 10-10 mutations/bp/cell division− 2 x 109 bp, so about one mistake (mutation) in
every 10 cell divisions of a stem cell)There is an intrinsic chemical instability of certain DNA bases that might give rise to mistakes or mutationsThe DNA can be attacked by free radicals, ionizing radiation, UV radiation, and chemical carcinogens—producing mutations
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Mutations
Finally, viruses, such as human papilloma virus (HPV), contain proteins that bind to and inhibit p53 and RB leading to an increase of genomic instability and an increase in mutations“Random mutations in the genes which control proliferation or apoptosis are responsible for Cancer”(Bertram, J.S. 2001. Molecular aspects of medicine. 21: 167-223.)
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Five Major Pathways: Cancer Cells
There are five major pathways that must be activated or inactivated in a cell for the cell to become a cancer cell− Growth stimulatory signals− Growth inhibitory signals− Apoptosis resistance− Infinite proliferative capacity− Angiogenic potential
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How Is Cancer Studied in the Laboratory?
Cancer in “cell culture”—transformed cellsNormal cells and transformed cells differ in:− Morphology− Contact inhibition− Serum (growth factor) dependence− Anchorage dependence− Tumorigenicity
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Tumor Cells and Viruses
Tumor cells contained a “cancer” geneTumor viruses contained “cancer” genes (oncogenes), which had cellular counterparts− Over 25 distinct cellular genes, now referred to as
proto-oncogenes, have been identifiedOncogenes are involved in signaling pathways that increase proliferation
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The Proto-Oncogene
Often the presence of the proto-oncogene is not sufficient to cause cancerHowever, increased expression of the proto-oncogene may cause cancerGenomic instability or the integration of retroviruses may give rise to cancer by increasing the expression of proto-oncogenesTumors have chromosomal abnormalities− Gain and loss of chromosomes, translocation, and
amplifications
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Section B
Oncogenes
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B Cell Tumors
Many B cell tumors carry chromosomal translocations that join the c-myc proto-oncogene to one of the immuno-globulin genes
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Oncogenes and Tumor Viruses
Oncogenes were isolated from tumor viruses, and they were also isolated from tumor tissueThe oncogenes from viruses and tumor tissue were not always precisely the same as the proto-oncogene
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Section C
Tumor Suppressor Genes
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Rapid Progress in the Field of Oncogenes
One of the reasons that progress was rapid in the field of oncogenes was that the addition of oncogenes to cells was genetically dominantHowever, in some experiments using cancer cells in culture, the tumorigenicity phenotype was recessive to normal growth
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Growth-Suppressing Genes
These experiments led to the idea that cells had growth-suppressing genes− If these genes were inactivated by mutation or
deletion, then cancer would resultThere are numerous tumor-suppressor genes and anti-oncogenesThese tumor suppressor genes code for proteins that normally act as checkpoints to cell proliferations or cell death
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Retinoblastoma (RB) Susceptibility Gene
One of these tumor suppressor genes is the retinoblastoma (RB) susceptibility geneThis gene was isolated by positional cloningIt was known that retinoblastoma, tumors of the eye in children, were associated with deletion of 13q14.11Probes to this region of chromosome 13 were isolatedRegions of chromosome 13 near this region were tested for expression as mRNA, presence of closely related sequences in other species (mouse, rat, etc.), and deleted, rearranged, or mutated DNA of retinoblastoma cells
Continued
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Retinoblastoma (RB) Susceptibility Gene
Another tumor suppressor gene, p53, was first isolated because a mutated form of p53 was a dominantly acting oncogeneMutation in p53 are now known to be associated with increased susceptibility to cancer
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Some Presumptive Suppressor Genes
RB− Chromosome 13q
Wilms tumor gene WT1− Chromosome 11p
Deleted colon carcinoma, DCC− Chromosome 18q
Neurofibromatosis gene type 1 NF1− Chromosome 17q
P53− Chromosome 17q
Gene involved in familial adenomatous polyposis coli, APC− Chromosome 5q
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Li-Fraumeni Syndrome
A mutant p53 gene is responsible for inherited cancers in the Li-Fraumeni syndrome
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Section D
Cancer Is a Multigenic Disease
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Causes of Cancer
Cancer is caused by mutations in many genes
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Some Questions
What do cancer genes code for? what processes are altered that give rise to cancer?− Signal transduction− Cell cycle checkpoints− DNA repair− Balance between cell division and apoptosis− Angiogenesis
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Molecular Diagnosis
My vision for the future is that we will no longer be diagnosed with breast cancer or prostate cancer or brain cancer—but rather with a cancer having the following genes malfunctioningThis approach to diagnosis—having a molecular diagnosis—will then allow us to tailor the treatment of the individual
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Section E
Therapies
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Potential and Actual Therapies
SurgeryConventional chemotherapyRadiation therapyHormone therapyMonoclonal antibodiesAntibody toxin conjugatesAntibody radionucleotide therapyPatient-specific vaccines
ImmunotherapySpecific protein kinase inhibitorsGene therapyVirotherapy (October 2003 Scientific American)Antisense therapyAnti-angiogenesis therapy
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Gleevec
Remember we talked about the fusion between BCR gene and the ABL geneThe result was the p210 BCR-ABL protein—that is a new protein kinaseDrug STI-571 (Gleevec) was developed as an inhibitor of the BCR-ABL proteinThe drug was effective in early-stage disease, but resistance developed in blast-stage diseaseThe mechanism of resistance was a single mutation in p210 or an increase in the BCR-ABL gene number
Reference: Nature, 2001. 412 pp. 281–282.
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Retinoblastoma (Rb) Protein
Cell-cycle master switch− Implicated in DNA replication, differentiation, DNA
repair, cell-cycle checkpoints, and apoptosisInteracts with many (over 100?) different cellular proteins—for example:− Cyclin-dependent kinases (phosphorylate Rb to
turn on cell proliferation)− E2F, a transcription factor, to sequester it
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Protein Kinases ATM and ATR
Part of the DNA damage response pathway (DRP)DRP controls DNA repair, telomerase composition and length, transcriptional programs, and apoptosisDRP proteins sense damage, transduce the damage signal, and affect a responseDRP includes:− p53, ATM, BRCAI, Rad 55, ChKl, and ChK2.
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Deranged Pathways
Spaghetti Junction
The pathways that, when deranged, lead to cancer are complex, interconnected, and many. This table lists some of the better-understood ones.
Additional Pathways Perturbed in Cancer
Representative Cancer Types
WNT/Beta-catenin/APC Colorectal cancer, melanoma Transforming Growth Factor-b (TGF-b) Hereditary nonpolyposis colon cancer,
gastrointestinal, prostate, ovarian cancer
Ras Hematopoietic, breast, ovarian, pancreatic, bladder cancer
c-Myc Breast, bladder, B cell leukemia, melanoma, and many more
Notch Hematopoietic cancer Jak/Stat Hematopoietic cancer Nfkb Hematopoietic cancer BCR-ABL molecular defect Chronic myelogenous leukemia Sonic hedgehog/Patched Basal cell carcinoma Epidermal Growth Factor Receptor (EGFR) Breast cancer, lung cancer,
ameloblastoma, many other cancers of epithelial origin
Telomerase Expression Multiple human cancers
Schultz, L.B., September 22, 2003. Aberrant signaling, The Scientist, 10–12.
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Section F
Cancer and Genomics
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Recent Strategies
Recent strategies for studying cancer that involve analysis of multiple samples− Genomics: high-throughput technologies for
analyzing genes− Transcriptomics: high-throughput technologies for
analyzing messenger RNAs− Proteomics: high-throughput technologies for
analyzing proteins
Reference: Olli Kallioniemi, March 25, 2004. Profile of a tumor. Nature; 428, pp. 379–382.
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An Example of Genomics
An example of genomics would be:− An experiment analyzing the expression of 70
informative genes in breast tumors to associate the messenger RNA expression of certain of these genes to good or poor prognosis
References: van’t Veer, L.J., et al. 2002. Nature 514, 530–536.Van de Vijver, M.J., et al. 2002. N. Engl. J. Med. 347, 1999–2009.
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Outcome
The outcome of this genomic study would be to help clinicians distinguish between:− Those women having breast tumors who have a
poor prognosis and might need adjuvant therapy or chemotherapy
− Those women who have a good prognosis—whereby some of those treatments may not be necessary
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Proteomics
Proteomics− An analysis of blood serum using mass
spectrometry to identify up to 15,000 peaks, which represent fragments of protein that are defined by their mass-to-charge ratios
Purpose of this technology− To determine if there are tumor markers for certain
cancers that show up in the blood
Continued
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Proteomics
Proteomics− Analysis of levels of specific phosphorylated
proteins in tumor samplesPurpose of this technology− This analysis is to determine correlations of certain
signaling pathways in tumors that might help target inhibitor studies
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Mutations Leading to Cancer
It is known that mutations in about 1% of human genes (a total of about 290 genes) are reported to contribute to cancerIt is estimated that there are around 500 new anticancer drugs currently in clinical trials
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Section G
Multidrug Resistance and Cancer
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Multidrug Resistance and Cancer
Multidrug resistance (MDR) in human malignancies is likely to be a major cause of failure in cancer chemotherapyCharacterization of independently derived MDR cell lines clearly illustrates that MDR can be mediated by the overproduction of a 170 kDa glycosylated plasma membrane protein called P-glycoprotein− “P” in this case stands for permeability
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How Can a Cell Become Drug Resistant?
Decreased uptakeIncreased degradationIncreased efflux of the drugAll of these mechanisms can be imagined for a particular drug, but the unique thing about MDR is that it is characterized by simultaneous acquisition of resistance to drugs that are structurally and functionally unrelated− The cells become resistant to a number of
unrelated drugs by a selection protocol to a single cytotoxic drug
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Characteristics of the Chemotherapy Drugs
Characteristics of the chemotherapy drugs− Predominantly alkaloids− Antibiotics of plant and fungal origin
Resistance to these compounds is thought to be achieved by lowered intracellular drug concentration: increased efflux
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Overproduction of the P-glycoprotein
Overproduction of the P-glycoprotein is caused by a gene amplification event: 100–200 copies of gene
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Points
Amplification of CHP1 homologous sequences correlated with MDR− Areas of up to 500 kb are amplified up to
100–200 timesHighly resistant cells have karyotypic changes:− HSR (homogeneously staining regions)
Staining with Giemsa− Double minute chromosomes− Chromosome translocations
Continued
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Points
This 600 bp sequence with no internal Eco R1 sites detected multiple bands− One indication that P-glycoprotein is encoded by a
multigene familyHamster probe could hybridize to mouse and human
Conserved nucleotide sequences
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P-glycoprotein
P-glycoprotein is also found widespread in human cancers− Including leukemias, lymphomas, sarcomas, and
carcinomasMDR cell lines can be isolated from drug-sensitive tumor cells
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Resistance of Human Tumors to Chemotherapy
Resistance of human tumors to chemotherapy follows a similar pattern in two situations:− For many tumors (adenocarcinomas of the colon
and kidney), malignant cells are primarily unresponsive to multiple chemotherapeutic agents (intrinsic drug resistance)
− In other cases (childhood leukemias and neuroblastomas), there is a good response initially to chemotherapy but tumors become refractory to therapy (acquired drug resistance)
Drugs of proven chemotherapeutic value include vinblastine, daunorubicin, and actinomycin D
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Potential Clinical Implications
If MDR is found (using cDNA probes for mRNA levels of MDR1 gene), then non-toxic drugs able to reverse the multidrug resistance phenotype might be useful in converting drug-resistant tumors to drug-responsive tumorsAntibody against P-glycoprotein linked to toxin will specifically kill multidrug resistant cell lines
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“An Ideal World” versus “The Real Cellular World”
“In an ideal world, cell division, survival, and death are in sync, promoting homeostasis with neither unregulated growth nor inappropriate cell loss. However, the real cellular world is laden with oncogenes and tumor suppressor genes whose products interact in overlapping pathways that, when dysfunctional, can lead to cancer.”
Source: The Scientist, September 22, 2003, pp. 10–12.