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==Pathology simplified== | ==Pathology simplified== | ||
===Blue & pink=== | |||
H&E is the standard... | H&E is the standard... | ||
*Too much '''PINK''' = DEAD ([[necrosis]]). | *Too much '''PINK''' = DEAD ([[necrosis]]). | ||
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In words: | In words: | ||
*''Blue is bad and pink is dead!''<ref> | *''Blue is bad and pink is dead!''<ref>Streutker, C. 8 June 2013.</ref> | ||
Note: | Note: | ||
*Lymph | *There is a lengthy list of things that are blue and ''not'' "bad"... that why a pathology residency is years. | ||
**[[Lymph node]]s are very blue... they aren't necessarily bad. | |||
**Reactive processes can be very blue... they aren't bad. | |||
===Three questions=== | |||
Pathology can be boiled down to: | |||
#What is it? | |||
#*Biopsies. | |||
#Did I get it all? | |||
#*Resections. | |||
#Did I get the right thing? | |||
#*Most other things. | |||
==Terms== | ==Terms== | ||
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*''Argyrophilic'' means has an affinity for silver<ref>URL: [http://www.merriam-webster.com/medical/argyrophilic http://www.merriam-webster.com/medical/argyrophilic]. Accessed on: 29 August 2011.</ref><ref>URL: [http://en.wiktionary.org/wiki/argyrophilic http://en.wiktionary.org/wiki/argyrophilic]. Accessed on: 29 August 2011.</ref>/loves silver/stains with silver. | *''Argyrophilic'' means has an affinity for silver<ref>URL: [http://www.merriam-webster.com/medical/argyrophilic http://www.merriam-webster.com/medical/argyrophilic]. Accessed on: 29 August 2011.</ref><ref>URL: [http://en.wiktionary.org/wiki/argyrophilic http://en.wiktionary.org/wiki/argyrophilic]. Accessed on: 29 August 2011.</ref>/loves silver/stains with silver. | ||
===Morphologic patterns=== | ===Morphologic patterns=== | ||
{| | {{Main|Morphologic patterns}} | ||
This covers things like ''cribriform'', ''hobnail'', ''herring bone'' and many others. | |||
===Nuclear destruction words=== | ===Nuclear destruction words=== | ||
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*Ulcer = lesion through skin or mucous membrane. | *Ulcer = lesion through skin or mucous membrane. | ||
*Erosion = limited to the mucosa - superficial ulceration. | *Erosion = limited to the mucosa - superficial ulceration. | ||
**In dermatopathology - through the epidermis. | |||
Image: | |||
<gallery> | |||
Image:Ulcers,_fissures,_and_erosions.svg | Ulcers and erosions - schematic. (WC) | |||
</gallery> | |||
====Microscopic - erosion==== | ====Microscopic - erosion==== | ||
Features - require 1 and 2: | Features - require 1 and 2: | ||
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#*+/-Fibrin. | #*+/-Fibrin. | ||
#*+/-Cellular debris. | #*+/-Cellular debris. | ||
Image: | |||
*[http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3400158/figure/f4-cln_67p705/ Mucosal erosion (nih.gov)].<ref name=pmid22892912>{{Cite journal | last1 = Arashiro | first1 = RT. | last2 = Teixeira | first2 = MG. | last3 = Rawet | first3 = V. | last4 = Quintanilha | first4 = AG. | last5 = Paula | first5 = HM. | last6 = Silva | first6 = AZ. | last7 = Nahas | first7 = SC. | last8 = Cecconello | first8 = I. | title = Histopathological evaluation and risk factors related to the development of pouchitis in patients with ileal pouches for ulcerative colitis. | journal = Clinics (Sao Paulo) | volume = 67 | issue = 7 | pages = 705-10 | month = Jul | year = 2012 | doi = | PMID = 22892912 | PMC = 3400158 | URL = http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3400158/}}</ref> | |||
==The general differential diagnosis== | ==The general differential diagnosis== | ||
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*Benign soft tissue lesions may have marked [[nuclear atypia]] and abundant mitotic activity. | *Benign soft tissue lesions may have marked [[nuclear atypia]] and abundant mitotic activity. | ||
=== | ===General differential diagnosis of malignant lesion=== | ||
This should ''always'' be considered: | This should ''always'' be considered: | ||
<center> | <center> | ||
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Q. Why? <br> | Q. Why? <br> | ||
A. (1) The site of the tumour can considerably change the differential diagnosis. (2) The management is usually totally different.<br><br> | A. (1) The site of the tumour can considerably change the differential diagnosis. (2) The management is usually totally different.<br><br> | ||
A | |||
===A general clinico-histomorphologically motivated differential diagnosis of malignancy=== | |||
<center> | <center> | ||
<!-- | <!-- | ||
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{{familytree | | | | | | | | | | | A | | | | | | | | | | |A=Malignancy}} | {{familytree | | | | | | | | | | | A | | | | | | | | | | |A=Malignancy}} | ||
{{familytree | |,|-|-|-|v|-|-|-|v|-|^|-|v|-|-|-|v|-|-|-|.| |}} | {{familytree | |,|-|-|-|v|-|-|-|v|-|^|-|v|-|-|-|v|-|-|-|.| |}} | ||
{{familytree | B | | C | | D | | E | | F | |G |B=Epithelial<br>(Carcinoma)|C=Mesenchymal<br>(Sarcoma)|D=[[Germ cell tumours|Germ cell<br>tumour]]|E=[[Neuroendocrine carcinoma|Neuroendocrine<br>carcinoma]]|F=Hematologic|G=[[Melanoma|Malignant<br>melanoma]]}} | {{familytree | B | | C | | D | | E | | F | |G |B=Epithelial<br>(Carcinoma)|C=Mesenchymal<br>([[Sarcoma]])|D=[[Germ cell tumours|Germ cell<br>tumour]]|E=[[Neuroendocrine carcinoma|Neuroendocrine<br>carcinoma]]|F=Hematologic|G=[[Melanoma|Malignant<br>melanoma]]}} | ||
{{familytree/end}} | {{familytree/end}} | ||
</center> | </center> | ||
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*''[[Malignant melanoma]]'', also ''melanoma'', is a separate category as it can look like almost anything under the microscope. | *''[[Malignant melanoma]]'', also ''melanoma'', is a separate category as it can look like almost anything under the microscope. | ||
*''Hematologic'' includes [[lymphoma]], [[leukemia]], [[plasma cell neoplasms]] and others. | *''Hematologic'' includes [[lymphoma]], [[leukemia]], [[plasma cell neoplasms]] and others. | ||
*The above is a useful clinical classification. The problem is it isn't that useful for difficult cases as: | |||
**Germ cell tumours are often not distinctive. | |||
**Numerous epithelioid sarcomas can mimic carcinomas. | |||
**Spindle cell carcinomas can mimic sarcomas very well. | |||
**Neuroendocrine differentiation is not always readily apparent. | |||
**The ''[[modified general morphologic DDx of malignancy]]'' is better for approaching difficult tumours. | |||
Memory device ''HMN GEM'': hematologic, melanoma, neuroendocrine carcinoma, germ cell, epithelial, mesenchymal. | |||
===Morphologic | ====Morphologic categorization==== | ||
=====Factors to consider===== | |||
Factors to consider when attempting to group by morphology: | Factors to consider when attempting to group by morphology: | ||
#Cell shape (spindle cell, epithelioid, plasmacytoid, mixed). | |||
#Cell size (small or large) - size in relation to a neutrophil or [[red blood cell]]. | |||
#Cell cohesion - dyscohesive vs. cohesive. | #Cell cohesion - dyscohesive vs. cohesive. | ||
#*If one sees several groups of 5+ cells... probably cohesive. | #*If one sees several groups of 5+ cells... probably cohesive. | ||
#*Presence of cell cohesion strongly disfavours lymphoma. | #*Presence of cell cohesion strongly disfavours lymphoma. | ||
#Cytoplasm - abundance (scant, moderate, abundant). | #Cytoplasm - abundance (scant, moderate, abundant). | ||
#*Eosinophilic cytoplasm disfavours lymphoma. | #*Eosinophilic cytoplasm disfavours lymphoma. | ||
#*Oncocytic - possessing copious eosinophilic granular cytoplasm. | |||
#**Benign lesions composed of oncocytes - oncocytoma | |||
#**Oncocytic metaplasia (alteration of cytoplasm) can effect all or a part of a lesion. | |||
#**Oncocytic neoplasms are common in the kidneys, thyroid and salivary glands. | |||
#**Oncocytic change increases with age | |||
#**May represent senescent accumulation of mitochondria in secretory epithelial. | |||
#Chromatin - coarseness (fine, granular). | #Chromatin - coarseness (fine, granular). | ||
#Nucleoli - number (absent, present, multiple). | #Nucleoli - number (absent, present, multiple). | ||
#*Large [[nucleoli]] (nucleoli seen with the 10x objective) pretty much exclude neuroendocrine. | #*Large [[nucleoli]] (nucleoli seen with the 10x objective) pretty much exclude neuroendocrine. | ||
======Types of cells====== | |||
{| class="wikitable sortable" | |||
! Type | |||
! Morphology | |||
! Significance | |||
|- | |||
* | | [[Spindle cell]] | ||
| tapered at both ends<ref>URL: [http://www.medterms.com/script/main/art.asp?articlekey=25657 http://www.medterms.com/script/main/art.asp?articlekey=25657]. Accessed on: 18 January 2010.</ref> | |||
| suggestive of sarcoma - compatible with melanoma and some carcinomas | |||
|- | |||
| Epithelioid cell | |||
| cell shape round/oval, nucleus round/oval, looks like epithelium (cell borders touch neighbouring cells - collectively form a barrier) | |||
| suggests epithelial lesion (carcinoma) - compatible with others | |||
|- | |||
| [[Small round blue cell tumour]]/lymphoid: | |||
| small cells with scant cytoplasm - usually round; "small" is classically 2x a "resting lymphocyte" diameter † | |||
| common in children; in adults often lymphoma | |||
|- | |||
| Small lymphoid ([[small cell lymphoma]]). | |||
| "small" in the context of lymphoid is classically ~1x a "resting lymphocyte" diameter; often not malignant by cytology | |||
| suggests [[small cell lymphoma]], reactive changes or infection | |||
|- | |||
| Plasmacytoid cell | |||
| resemble a plasma cell: eccentric nucleus, moderate basophilic cytoplasm, +/-"clockface" chromatin pattern (clumping of chromatin at the periphery of the nucleus), +/-perinuclear hof (crescentic cytoplasmic clearing adjacent to the nucleus; represents abundant Golgi apparatus | |||
| suggests [[plasma cell neoplasm]] or infection | |||
|} | |||
Note: | |||
*† Diameter of a "resting lymphocyte" ~ diameter of a [[red blood cell]] (RBC) ~ 8 micrometres. | |||
**Most carcinoma cells are 3-4x the size of a RBC. | |||
====Dyscohesive | ======Dyscohesive versus cohesive====== | ||
Deciding cells are dyscohesive vs. cohesive is important, as it is a strong determinant of whether one is dealing with a lymphoid lesion or not. | Deciding cells are dyscohesive vs. cohesive is important, as it is a strong determinant of whether one is dealing with a lymphoid lesion or not. | ||
{| class="wikitable" | {| class="wikitable sortable" | ||
!| | !| | ||
!| Cell spacing | !| Cell spacing | ||
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*Basophilic cytoplasm. | *Basophilic cytoplasm. | ||
=== | =====Probable category by morphology===== | ||
*Carcinoma = cohesive, relatively large (>~2X neutrophil), +/-nucleolus, +/-gland formation (circular structures), often moderate to abundant cytoplasm. | |||
*Sarcoma = cohesive, composed of spindle cells (cells taper at both ends, nucleus oval/cigar-shaped). | |||
*Germ cell tumour = appearance often similar to ''carcinoma'', site (location) very useful - esp. gonadal, midline, retroperitoneal. | |||
* | *[[Neuroendocrine carcinoma]] = cohesive, fine granular chromatin and no [[nucleolus]]. | ||
*Lymphoma = dyscohesive, relatively small (usually <=2X neutrophil diameter), usu. scant basophilic (blue) cytoplasm. | |||
*Melanoma = classically pigmented, often a prominent [[red nucleolus]], a mix of spindle cells and epithelioid cells, mix of cohesive and dyscohesive cells. | |||
* | |||
* | ===A practical histomorphologic differential diagnosis of malignancy=== | ||
*[[ | ====General morphologic DDx of malignancy==== | ||
* | {{familytree/start}} | ||
* | {{familytree | | | | | | | A01 | | | | | | | | A01=Malignancy}} | ||
{{familytree | |,|-|-|-|v|-|^|-|v|-|-|-|.| | |}} | |||
{{familytree | B01 | | B02 | | B03 | | B04 | |B01=[[Large epithelioid tumours]]|B02=[[spindle cell lesions|Spindle cell tumours]]|B03=[[small round cell tumours|Small blue cell tumours]]|B04=[[Pleomorphic tumours]]}} | |||
{{familytree/end}} | |||
====Modified general morphologic DDx of malignancy==== | |||
<center> | |||
{{familytree/start}} | |||
{{familytree | | | | | | | | | | | A | | | | | | | | | | |A=Malignancy}} | |||
{{familytree | |,|-|-|-|v|-|-|-|v|-|^|-|v|-|-|-|v|-|-|-|.| |}} | |||
{{familytree | B | | C | | D | | E | | F | |G |B=[[Large epithelioid tumours]]|C=[[spindle cell lesions|Spindle cell tumours]]|D=[[small round cell tumours|Small blue cell tumours]]|E=[[Pleomorphic tumours]]|F=[[Clear cell tumours]]|G=[[myxoid lesions|Myxoid tumours]]}} | |||
{{familytree/end}} | |||
</center> | |||
The above is more useful than the ''general clinico-histomorphologically motivated differential diagnosis of malignancy''. | |||
==Differential diagnosis by site== | ==Differential diagnosis by site== | ||
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*Apoptotic cell -- has nuclear condensation (pyknosis), eosinophilic cytoplasm. | *Apoptotic cell -- has nuclear condensation (pyknosis), eosinophilic cytoplasm. | ||
Images: | ====Images==== | ||
<gallery> | |||
Image:Atypical_mitosis.jpg| Mitoses and an atypical mitosis. (WC) | |||
Image:Tripolar_Mitosis_-_breast_carcinoma.jpg| Tripolar mitosis. (WC) | |||
</gallery> | |||
www: | |||
*[http://education.vetmed.vt.edu/Curriculum/VM8054/Labs/Lab4/IMAGES/MITOSIS%20IN%20GUT.JPG Mitoses (vetmed.vt.edu)]. | *[http://education.vetmed.vt.edu/Curriculum/VM8054/Labs/Lab4/IMAGES/MITOSIS%20IN%20GUT.JPG Mitoses (vetmed.vt.edu)]. | ||
*[http://www.flickr.com/photos/euthman/426956752/ Starburst mitosis (flicker.com)]. | *[http://www.flickr.com/photos/euthman/426956752/ Starburst mitosis (flicker.com)]. | ||
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*A collection of PMNs... think about ''necrosis'' and ''abscess''. | *A collection of PMNs... think about ''necrosis'' and ''abscess''. | ||
===Lymph node | ===Lymph node metastasis=== | ||
{{Main|Lymph node metastasis}} | {{Main|Lymph node metastasis}} | ||
*Take a good to look at the tumour first. | *Take a good to look at the tumour first. | ||
*Tumour in a node is often better differentiated than the most poorly differentiated part in the primary site. | *Tumour in a node is often better differentiated than the most poorly differentiated part in the primary site. | ||
*Subcapsular space - the first place to look for mets. | *Subcapsular space - the first place to look for mets. | ||
*Lymph node | *Lymph node metastasis are usually obvious. | ||
**There are of course exceptions, e.g. [[small cell carcinoma]], [[invasive lobular carcinoma]]. | **There are of course exceptions, e.g. [[small cell carcinoma]], [[invasive lobular carcinoma]]. | ||
*Histiocytes may be difficult to separate from tumour - especially for the novice. | *Histiocytes may be difficult to separate from tumour - especially for the novice. | ||
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DDx: | DDx: | ||
*Fat atrophy. | *[[Fat atrophy]]. | ||
Stains: | Stains: | ||
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*Alican blue-PAS stain. | *Alican blue-PAS stain. | ||
Images: | ====Images==== | ||
<gallery> | |||
Image:Signet_ring_cells_5.jpg |SRCs - H&E stain. (WC/Nephron) | |||
Image:Gastric_signet_ring_cell_carcinoma_histopatholgy_(2)_PAS_stain.jpg | SRCs - AL-PAS stain. (WC) | |||
Image:Gastric_signet_ring_cell_carcinoma_histopatholgy_(1).jpg | SRC - H&E stain. (WC) | |||
</gallery> | |||
www: | |||
*[http://www.engravingarts.com/sales/LVX2.jpg Signet rings (engravingarts.com)]. | *[http://www.engravingarts.com/sales/LVX2.jpg Signet rings (engravingarts.com)]. | ||
===Necrosis=== | ===Necrosis=== | ||
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*[http://www.nature.com/bmt/journal/v39/n9/fig_tab/1705646f1.html Necrosis (nature.com)]. | *[http://www.nature.com/bmt/journal/v39/n9/fig_tab/1705646f1.html Necrosis (nature.com)]. | ||
*[http://moon.ouhsc.edu/kfung/jty1/Com08/Com08Image/Com801-1-09.gif Necrosis (ouhsc.edu)].<ref>URL: [http://moon.ouhsc.edu/kfung/jty1/Com08/Com801-1-Diss.htm http://moon.ouhsc.edu/kfung/jty1/Com08/Com801-1-Diss.htm]. Accessed on: 3 November 2010.</ref> | *[http://moon.ouhsc.edu/kfung/jty1/Com08/Com08Image/Com801-1-09.gif Necrosis (ouhsc.edu)].<ref>URL: [http://moon.ouhsc.edu/kfung/jty1/Com08/Com801-1-Diss.htm http://moon.ouhsc.edu/kfung/jty1/Com08/Com801-1-Diss.htm]. Accessed on: 3 November 2010.</ref> | ||
<gallery> | |||
Image:Cat_scratch_disease_-_very_high_mag.jpg | Necrosis in [[cat scratch disease]]. (WC/Nephron) | |||
Image:Histiocytic_necrotizing_lymphadenitis_-_very_high_mag.jpg | Necrosis in [[histiocytic necrotizing lymphadenitis]]. (WC/Nephron) | |||
Image:Systemic_lupus_erythematosus_lymphadenopathy_-_high_mag.jpg | Necrosis in [[SLE lymphadenopathy]]. (WC/Nephron) | |||
</gallery> | |||
==Granulomas== | ==Granulomas== | ||
{{Main|Granuloma}} | |||
==Common morphologic problems== | ==Common morphologic problems== | ||
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*'''S'''mooth muscle cells (SMCs). | *'''S'''mooth muscle cells (SMCs). | ||
Images: | =====Images===== | ||
<gallery> | |||
Image:Cardiac_amyloidosis_high_mag_he.jpg | Cardiac amyloid. (WC/Nephron) | |||
Image:Laminations_in_a_thrombus_-_high_mag.jpg | Fibrin in a thrombus. (WC/Nephron) | |||
Image:Ovarian_fibroma_-_high_mag.jpg | Collagen in an ovarian fibroma. (WC/Nephron) | |||
Image:Glatte_Muskelzellen.jpg | Smooth muscle. (WC/Polarlys) | |||
</gallery> | |||
====Smooth muscle cells (SMCs) vs. fibrous tissue==== | ====Smooth muscle cells (SMCs) vs. fibrous tissue==== | ||
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*Schwann cells (found in nerve): nuclei = wavy appearance, thin. (???) | *Schwann cells (found in nerve): nuclei = wavy appearance, thin. (???) | ||
=== | ===Pigmented material=== | ||
*[[AKA]] brown/black granular crap. | |||
DDx of granular stuff/pigment: | DDx of granular stuff/pigment: | ||
#Lipofuscin - especially in old people. | #Lipofuscin - especially in old people. | ||
#Hemosiderin. | #Hemosiderin. | ||
#Bile - found in hepatocytes, yellow. | #Bile - found in hepatocytes, yellow. | ||
#Foreign material (tattoo pigment, anthracotic pigment). | #Foreign material (tattoo pigment, anthracotic pigment, [[amalgam tattoo]]). | ||
#Melanin. | #Melanin. | ||
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Note: | Note: | ||
*Most | *Most modern [[microscope]]s, have an eye piece diameter of 22 mm. Therefore, the field diameter at 40 X is approximately 22 mm / 40 X ~= 0.55 mm and the field of view is pi/4*(0.55 mm)^2 = 0.2376 mm^2. | ||
==Pathology reports== | ==Pathology reports== | ||
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==Lab talk== | ==Lab talk== | ||
{{Main|Cutting}} | |||
Tissue cutting terms - these often vary from lab-to-lab:<ref>URL: [http://www.mailman.srv.ualberta.ca/pipermail/patho-l/2002-July/016955.html http://www.mailman.srv.ualberta.ca/pipermail/patho-l/2002-July/016955.html]. Accessed on: 18 October 2011.</ref> | Tissue cutting terms - these often vary from lab-to-lab:<ref>URL: [http://www.mailman.srv.ualberta.ca/pipermail/patho-l/2002-July/016955.html http://www.mailman.srv.ualberta.ca/pipermail/patho-l/2002-July/016955.html]. Accessed on: 18 October 2011.</ref> | ||
*Recut = cut off the top of the block. | *Recut = cut off the top of the block. |
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