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File:Squamous cells.jpg
File:Dysplastic cells.jpg

Dysplasia (from ancient Greek δυσ- dys-, "difficulty" + πλάσις plasis, "formation") is a term used in pathology to refer to an abnormality of development.[1] This generally consists of an expansion of immature cells (such as cells of the ectoderm), with a corresponding decrease in the number and location of mature cells. Dysplasia is often indicative of an early neoplastic process. The term dysplasia is typically used when the cellular abnormality is restricted to the originating tissue, as in the case of an early, in-situ neoplasm.

Dysplasia, in which cell maturation and differentiation are delayed, can be contrasted with metaplasia, in which cells of one mature, differentiated type are replaced by cells of another mature, differentiated type.

The terms hip dysplasia and fibrous dysplasia also refer to abnormal development, but at a more macroscopic level.

Examples[]

Examples of dysplasia include epithelial dysplasia of the cervix (cervical intraepithelial neoplasia – a disorder commonly detected by an abnormal pap smear) consists of an increased population of immature (basal-like) cells which are restricted to the mucosal surface, and have not invaded through the basement membrane to the deeper soft tissues. Analogous conditions include vaginal intraepithelial neoplasia and vulvar intraepithelial neoplasia.

Myelodysplastic syndromes, or dysplasia of blood-forming cells, show increased numbers of immature cells in the bone marrow, and a decrease in mature, functional cells in the blood.

Screening[]

Some tests which detect cancer could be called "screening for dysplasia". The principle behind these tests is that physicians expect dysplasia to occur at the same rate in a typical individual as it would in many other people. Because of this, researchers design screening recommendations which assume that if a physician can find no dysplasia at certain time, then doing testing before waiting until new dysplasia could potentially develop would be a waste of medical resources for the patient and the healthcare provider because the chances of detecting anything is extremely low.

Some examples of this in practice are that if a patient whose endoscopy did not detect dysplasia on biopsy during screening for Barrett's esophagus, then research shows that there is little chance of any test detecting dysplasia for that patient within three years.[2][3][4]

Individuals at average-risk for colorectal cancer should have another screening after ten years if they get a normal result and after five years if they have only 1-2 adenomatous polyps removed.[2][5][6][7]

Microscopic changes[]

Dysplasia is characterised by four major pathological microscopic changes:

  1. Anisocytosis (cells of unequal size)
  2. Poikilocytosis (abnormally shaped cells)
  3. Hyperchromatism (excessive pigmentation)[8]
  4. Presence of mitotic figures (an unusual number of cells which are currently dividing).[9]

Dysplasia vs. carcinoma in situ vs. invasive carcinoma[]

File:Blausen 0221 CervicalDysplasia.png

Cervical Dysplasia illustrations showing CIN pathology.

These terms are related since they represent the three steps in the progression of many malignant neoplasms (cancers) of epithelial tissues. The likelihood of developing carcinoma is related to the degree of dysplasia.[10]

  • Dysplasia is the earliest form of pre-cancerous lesion which pathologists can recognize in a pap smear or in a biopsy. Dysplasia can be low grade or high grade (see "Carcinoma in situ" below). The risk of low grade dysplasia transforming into high grade dysplasia, and eventually cancer, is low. Treatment is usually straightforward. High grade dysplasia represents a more advanced progression towards malignant transformation.
  • Carcinoma in situ, meaning "cancer in place", represents the transformation of a neoplastic lesion to one in which cells undergo essentially no maturation, and thus may be considered cancer-like. In this state, epithelial cells have lost their tissue identity and have reverted to a primitive cell form that grows rapidly and with abnormal regulation for the tissue type. However, this form of cancer remains localized, and has not invaded past the basement membrane into tissues below the surface.
  • Invasive carcinoma is the final step in this sequence. It is a cancer which has invaded beyond the basement membrane and has potential to metastasize (spread to other parts of the body). Invasive carcinoma can usually be treated, but not always successfully. However, if it is left untreated, it is almost always fatal.

See also[]


Notes[]

  1. REDIRECT Template:Reflist


References[]

  • Noel Weidner (editor), Richard Cote, Saul Suster, Lawrence Weiss (2003). Modern Surgical Pathology, London: W.B. Saunders.
  • Ramzi S. Cotran, Vinay Kumar, Tucker Collins (Editor) (1999). Robbins Pathologic Basis of Disease, 6th, London: W.B. Saunders.



This page uses Creative Commons Licensed content from Wikipedia (view authors).
  1. Template:DorlandsDict
  2. 2.0 2.1 American Gastroenterological Association, Five Things Physicians and Patients Should Question, American Gastroenterological Association, http://choosingwisely.org/wp-content/uploads/2012/04/5things_12_factsheet_AGA.pdf, retrieved on August 17, 2012 
  3. PMID 21376940 (PMID 21376940)
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  4. PMID 18341497 (PMID 18341497)
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  5. PMID 12557158 (PMID 12557158)
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  6. PMID 16635231 (PMID 16635231)
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  7. PMID 18384785 (PMID 18384785)
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  8. Definition: hyperchromatic from Online Medical Dictionary. URL accessed on 2008-10-18.
  9. Abrams, Gerald Neoplasia I. URL accessed on 24 January 2012.
  10. Ridge JA, Glisson BS, Lango MN, et al. "Head and Neck Tumors" in Pazdur R, Wagman LD, Camphausen KA, Hoskins WJ (eds.) Cancer Management: A Multidisciplinary Approach. 11th ed. 2008.
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