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Although poorly differentiated [[tumors]] tend to behave more aggressively, well-differentiated [[tumors]] can also give rise to [[metastasis]] and result in death. Several [[histological]] variants of [[squamous cell carcinoma]] have been documented, including [[Verrucous carcinoma|verrucous]], [[Spindle cells|spindle cell]] and [[pseudovascular]].
Although poorly differentiated [[tumors]] tend to behave more aggressively, well-differentiated [[tumors]] can also give rise to [[metastasis]] and result in death. Several [[histological]] variants of [[squamous cell carcinoma]] have been documented, including [[Verrucous carcinoma|verrucous]], [[Spindle cells|spindle cell]] and [[pseudovascular]].
Frequently an [[actinic keratosis]] or [[squamous cell carcinoma]] overlies the [[invasive]] component and the two are focally [[contiguous]]. Occasionally [[squamous]] [[tumors]] arise rapidly, have a crater-form morphology and spontaneously regress. These [[tumors]] are known as [[Keratoacanthoma|keratoacanthomas]]. Some craterform [[squamous]] lesions do not [[Regression|regress]], but continue to invade and grow and represent [[invasive]] [[squamous cell carcinomas]].


=== Microscopic Pathology ===
=== Microscopic Pathology ===
[[Histopathological|Histopathological examination]] confirms diagnosis and aids in the [[Staging (pathology)|staging]] of the [[disease]]. [[Histopathological|Histopathology]] evaluates in detail the following characteristics :
*  
 
 
*[[Invasion]]
*[[Differentiation]]
*Depth
 
The various types of [[biopsy]] that may be obtained includes shave, punch, and [[Excisional biopsy|excisional biopsies]]. The sample may be obtained at a physician's office under [[local anesthesia]]. The type of [[biopsy]] method chosen is based upon the size of lesion.
*For smaller lesions in easy accessible region of the body, an [[excisional biopsy]] is preferred. This may be [[therapeutic]] as well as [[diagnostic]].
*For lesions which are large and for which the [[Cosmetics|cosmetic]] appearance may be of concern, a [[punch biopsy]] is advisable. Further treatment is based upon the results of [[Histopathological|histopathological evaluation]].
*A shave [[biopsy]] is seldom recommended in cases where the lesion is suspected to be [[malignant]].
 
Important principles to consider when taking a sample for [[biopsy]].
* A full thickness [[biopsy]] should be taken to best evaluate the true depth of the [[Lesions|lesion]] and extent of [[invasion]]. Depth of the lesion is an important determinant in the [[prognosis]] and [[Cancer staging|staging]] of [[Cancer (disease)|cancer]].<ref>Brantsch KD, Meisner C, Schönfisch B, Trilling B, Wehner-Caroli J, Röcken M, et al. Analysis of risk factors determining prognosis of cutaneous squamous-cell carcinoma: a prospective study. Lancet Oncol. Aug 2008;9(8):713-20</ref>
* The [[biopsy]] specimen should also include samples of normal [[tissue]] as a comparison.
* Large [[lesions]] require a thorough sample that will adequately assess the entirety of the [[Lesions|lesion]].'''<u>Findings</u>''' [[Histopathological|Histopathological evaluation]] is important in determining the next step in the [[Grading (tumors)|grade]] and treatment of the [[Cancer (medicine)|cancer.]] The [[Neoplastic|neoplastic cells]] may demonstrate varying degrees of [[squamous]] [[differentiation]] and [[atypia]] uncder the [[Microscopes|microscope]].  
* Large [[lesions]] require a thorough sample that will adequately assess the entirety of the [[Lesions|lesion]].'''<u>Findings</u>''' [[Histopathological|Histopathological evaluation]] is important in determining the next step in the [[Grading (tumors)|grade]] and treatment of the [[Cancer (medicine)|cancer.]] The [[Neoplastic|neoplastic cells]] may demonstrate varying degrees of [[squamous]] [[differentiation]] and [[atypia]] uncder the [[Microscopes|microscope]].  



Revision as of 17:50, 7 June 2019

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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Aditya Govindavarjhulla, M.B.B.S. [2], Raviteja Guddeti, M.B.B.S. [3]

Overview

Squamous cell carcinoma (SCC) is type of non-melanoma skin cancer. The cancer arises as a result of uncontrolled growth of the squamous cells in the epidermis of the skin. Unlike it's counter part, the basal cell carcinoma which also belongs to the group of non-melanoma cancer, squamous cell carcinoma is rapid growing and invasive. SCCs may occur on all areas of the body including the mucous membranes and genitals, but are most common in areas frequently exposed to the sun, such as the rim of the ear, lower lip, face, bald scalp, neck, hands, arms and legs. Wrinkling, changes in pigmentation, and loss of elasticity of the skin are often the telltale signs of sun damage.

Pathophysiology

Squamous cell carcinoma is a potentially invasive cancer that arises from the surface epithelium.The development of squamous cell carcinoma is frequently a multistep process. Early lesions tend to be either actinic keratoses, with atypia of the basal keratinocytic layer of the epidermis or squamous cell carcinoma in situ, in which keratinocytic atypia spans the full thickness epidermis.

These precursors are frequently present adjacent to invasive squamous cell carcinomas which invade the dermis as nests, islands, or cords squamous cells with or occasionally as individual cells. Several grading schemes have been developed for squamous cell carcinoma and incorporate the extent of keratinization (a form of differentiation) and nuclear atypia. A widely used scheme divides tumors into well, moderately, or poorly differentiated.

Although poorly differentiated tumors tend to behave more aggressively, well-differentiated tumors can also give rise to metastasis and result in death. Several histological variants of squamous cell carcinoma have been documented, including verrucous, spindle cell and pseudovascular.

Microscopic Pathology


References

  1. Ortonne JP (April 2002). "From actinic keratosis to squamous cell carcinoma". Br. J. Dermatol. 146 Suppl 61: 20–3. PMID 11966728.
  2. Berner A (June 2005). "[Actinic keratosis and development of cutaneous squamous cell carcinoma]". Tidsskr. Nor. Laegeforen. (in Norwegian). 125 (12): 1653–4. PMID 15976832.
  3. Tsai KY, Tsao H (November 2004). "The genetics of skin cancer". Am J Med Genet C Semin Med Genet. 131C (1): 82–92. doi:10.1002/ajmg.c.30037. PMID 15468170.
  4. Borelli D, Salas J (1975). "[The use of trypan blue instead of cotton blue in mycology]". Rev. Latinoam. Microbiol. (in Spanish; Castilian). 17 (3): 185–6. PMID 52880.
  5. Strabala TJ, Bednarek SY, Bertoni G, Amasino RM (April 1989). "Isolation and characterization of an ipt gene from the Ti plasmid Bo542". Mol. Gen. Genet. 216 (2–3): 388–94. PMID 2747621.
  6. Spencer JM, Kahn SM, Jiang W, DeLeo VA, Weinstein IB (July 1995). "Activated ras genes occur in human actinic keratoses, premalignant precursors to squamous cell carcinomas". Arch Dermatol. 131 (7): 796–800. PMID 7611795.
  7. Khavari PA (April 2006). "Modelling cancer in human skin tissue". Nat. Rev. Cancer. 6 (4): 270–80. doi:10.1038/nrc1838. PMID 16541145.


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