(pathology) An abnormally small G-group chromosome found in the hematopoietic cells of most patients with chronic granulocytic leukemia.
Philadelphia chromosome
| Sci-Tech Dictionary: Philadelphia chromosome |
(¦fil·ə¦del·fyə ′krō·mə′skōp)
| 5min Related Video: Philadelphia chromosome |
| Medical Dictionary: Phil·a·del·phi·a chromosome |
(fĭl'ə-dĕl'fē-ə)
n.
n.
An abnormal minute chromosome found in white blood cells in many cases of chronic myelocytic leukemia.
| Veterinary Dictionary: Philadelphia chromosome |
The 9:22 chromosomal translocation characterisitic of human patients with inherited predilection for chronic myelogenous leukemia.
| Wikipedia: Philadelphia chromosome |
| Philadelphia chromosome | |
|---|---|
| Classification and external resources | |
 A metaphase cell positive for the bcr/abl rearrangement using FISH |
|
| ICD-10 | C92.1 |
| ICD-9 | 205.1 |
| ICD-O: | 9875/3 |
| MeSH | D010677 |
Philadelphia chromosome or Philadelphia translocation is a specific chromosomal abnormality that is associated with chronic myelogenous leukemia (CML). It is the result of a reciprocal translocation between chromosome 9 and 22, and is specifically designated t(9;22)(q34;q11). The presence of this translocation is a highly sensitive test for CML, since 95% of people with CML have this abnormality (the remainder have either a cryptic translocation that is invisible on G-banded chromosome preparations, or a variant translocation involving another chromosome or chromosomes as well as the long arm of chromosomes 9 and 22). However, the presence of the Philadelphia (Ph) chromosome is not sufficiently specific to diagnose CML, since it is also found in acute lymphoblastic leukemia[1] (ALL, 25–30% in adult and 2–10% in pediatric cases) and occasionally in acute myelogenous leukemia (AML).
Contents |
Molecular biology
The exact chromosomal defect in Philadelphia chromosome is a translocation. Parts of two chromosomes, 9 and 22, swap places. The result is that a fusion gene is created by juxtapositioning of a part of the BCR ("breakpoint cluster region") gene from chromosome 22 (region q11) to the Abl1 gene on chromosome 9 (region q34).[2] In agreement with the International System for Human Cytogenetic Nomenclature (ISCN), this chromosomal translocation is designated as t(9;22)(q34;q11). Abl stands for "Abelson", the name of a leukemia virus which carries a similar protein.
The result of the translocation is the BCR-Abl gene, which is located on the shorter chromosome 22. BCR-Abl is a chimeric oncogene which encodes the protein p210 or sometimes p185 ("p" stands for protein and the numbers represent the molecular weight of the protein in kDa). Because the Abl gene expresses a membrane-associated protein, a tyrosine kinase, the BCR-Abl transcript is also translated into a tyrosine kinase, adding a phosphate group to tyrosine. Although the BCR region also expresses serine/threonine kinases, the tyrosine kinase function is very relevant for drug therapy. Tyrosine kinase inhibitors (such as imatinib and sunitinib) are important drugs against a variety of cancers including CML, RCC and GISTs. P210 occurs primarily in CML, and sometimes in Ph-positive acute lymphoblastic leukemia (Ph+ALL), for which the P190 protein is more common. For pediatric Ph+ALL, the impact of this type of fusion gene on prognosis after therapy is unknown since Ph+ALL is rare and to populate statistically relevant studies is difficult.
The fused BCR-Abl protein interacts with the interleukin-3 receptor beta(c) subunit. The BCR-Abl transcript is constitutively active, i.e. it does not require activation by other cellular messaging proteins. In turn, BCR-Abl activates a number of cell cycle-controlling proteins and enzymes, speeding up cell division. Moreover, it inhibits DNA repair, causing genomic instability and potentially causing the feared blast crisis in CML.
Nomenclature
Philadelphia chromosome is designated Ph (or Ph') chromosome and the translocation is termed t(9;22)(q34.1;q11.2).
Therapy
In the late 1990s, STI-571 (imatinib, Gleevec/Glivec) was identified by Novartis pharmaceuticals in high-throughput screens for tyrosine kinase inhibitors. Subsequent clinical trials led by Dr. Brian J. Druker at Oregon Health & Science University in collaboration with Dr. Charles Sawyers and Dr. Moshe Talpaz demonstrated that STI-571 inhibits proliferation of BCR-ABL-expressing hematopoietic cells. Although it did not eradicate CML cells, it did greatly limit the growth of the tumor clone and decreased the risk of the feared "blast crisis". In 2000 John Kuriyan determined the mechanism by which STI-571 inhibits the Abl kinase domain.[3] It was marketed in 2001 by the pharmaceutical company Novartis as imatinib mesylate (Gleevec in the US, Glivec in Europe). Other pharmacological inhibitors are being developed, which are more potent and/or are active against the emerging Gleevec/Glivec resistant BCR-abl clones in treated patients. The majority of these resistant clones are point-mutations in the kinase of BCR-abl. New inhibitors include dasatinib and nilotinib, which are significantly more potent than imatinib and may overcome resistance.
Treatment of pediatric Ph+ ALL with a combination of standard chemotherapy and RTK inhibitors may result in remission, but the curative potential is unknown. COG study AALL 0031, which examines the use of Gleevec with standard chemotherapeutic regimens and bone marrow transplant from HLA-matched related donors for high risk ALL (including PH+ ALL), has concluded, and findings will be published in the near future. A potentially curative, but risky option for pediatric PH+ ALL or PH+ CML includes bone marrow transplant or cord blood transplant, but chemotherapy is favored by some for achieving first remission (CR1). For some, bone marrow transplant from a matched sibling donor or a matched, unrelated donor may be favored when remission is obtained. Cord blood transplant is favored by some when a 10/10 bone marrow match is not available, and cord blood transplant may have some advantages, including a reduced incidence of graft-vs-host disease (GVHD), which is a common and significant complication of transplant. However, transplant with cord blood sometimes requires longer periods of time for engraftment, which may increase the potential for complications due to infection. Regardless of the type of transplant, transplant-related mortality and relapse are possible, and the rates may change as treatment protocols improve. For second remission (CR2), if achieved, both chemotherapy and transplant options are possible, and many physicicans prefer transplant.
History
The Philadelphia chromosome was first discovered and described in 1960 by Peter Nowell from University of Pennsylvania School of Medicine[4] and David Hungerford from the Fox Chase Cancer Center's Institute for Cancer Research and was therefore named after the city in which both facilities are located.
In 1973, Janet D. Rowley at the University of Chicago identified the mechanism by which the Philadelphia chromosome arises as a translocation.[5]
See also
- Refer to the article on Chronic myelogenous leukemia for more details on diagnosis and treatment.
- Chromosomal translocation
References
- ^ Talpaz M, Shah NP, Kantarjian H, et al. (June 2006). "Dasatinib in imatinib-resistant Philadelphia chromosome-positive leukemias". N. Engl. J. Med. 354 (24): 2531–41. doi:. PMID 16775234. http://content.nejm.org/cgi/pmidlookup?view=short&pmid=16775234&promo=ONFLNS19.
- ^ Kurzrock R, Kantarjian HM, Druker BJ, Talpaz M (May 2003). "Philadelphia chromosome-positive leukemias: from basic mechanisms to molecular therapeutics". Ann. Intern. Med. 138 (10): 819–30. PMID 12755554. http://www.annals.org/cgi/pmidlookup?view=long&pmid=12755554.
- ^ Schindler T, Bornmann W, Pellicena P, Miller WT, Clarkson B, Kuriyan J (2000). "AStructural mechanism for STI-571 inhibition of abelson tyrosine kinase". Science 289 (5486): 1857–9. doi:. PMID 10988075. http://www.sciencemag.org/cgi/content/full/289/5486/1938.
- ^ Nowell P, Hungerford D. "A minute chromosome in chronic granulocytic leukemia." Science 1960;132:1497.
- ^ Rowley JD (1973). "Letter: A new consistent chromosomal abnormality in chronic myelogenous leukaemia identified by quinacrine fluorescence and Giemsa staining". Nature 243 (5405): 290–3. doi:. PMID 4126434.
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