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==Overview==
==Overview==
Most clinically significant cases of non-puerperal mastitis start as [[inflammation]] of the ductal and [[lobular]] system and possibly the immediate surrounding [[tissue]]. Development of non-puerperal mastitis is the result of secretory [[stasis]] whereas puerperal mastitis occurs when [[bacteria]], often from the patient's [[skin]] or the baby's [[mouth]]/[[nostrils]],<ref>{{cite journal | title=A case-control study of mastitis: nasal carriage of ''Staphylococcus aureus'' | author=Amir LH, Garland SM, Lumley J. | journal=BMC Family Practice. | year=2006 | volume=7 | pages=57 | doi=10.1186/1471-2296-7-57}}</ref> enters a [[milk]] [[duct]] through a crack in the [[nipple]].


==Pathophysiology==
==Pathophysiology==
===Nonpuerperal Mastitis: Pathogenesis===
Most clinically significant cases of nonpeurperal mastitis start as inflammation of the ductal and lobular system (galactophoritis) and possibly the immediately surrounding tissue.
Development of Nonpeurperal mastitis is the result of Secretory stasis about 80% of cases. The retained secretions can get infected or lead to [[inflammation]] by causing mechanical damage or leaking the [[lactiferous duct]]s.
[[Autoimmune]] reaction to the [[secretion]]s may be also a factor.


Several mechanisms are thought to lead to the pathogenesis of mastitis are shown below:
* Secretory disease or [[galactorrhea]].
* Changes in [[permeability]] of lactiferous ducts (retention syndrome).
* Blockage of lactiferous ducts, for example duct plugging caused by squamous [[metaplasia]] of lactiferous ducts.
* Trauma, injury.
* Mechanical irritation caused by [[retention syndrome]] or [[Fibrocystic]] Condition.
* [[Infection]].
* Autoimmune reaction to luminal fluid.


About 25% of patients may be [[hyperprolactinemia|hyperprolactinemic]] and significant coincidence with [[fibrocystic breast disease|fibrocystic condition]] and [[thyroid]] anomalies has been documented (Peters & Schuth 1989, Goepel & Pahnke 1991). Up to 50% of patients experience transient [[hyperprolactinemia]] possibly caused by the [[inflammation]] or treatment and most had abnormally high [[Prolactin]] reserve (Goepel & Pahnke 1991).  
===Anatomy of the breast===
The images below show a general overview of [[breast]] [[anatomy]].


[[Prolactin]], [[IGF-1]] and [[TSH]] are important sytemic factors in galactopoiesis, their significance in secretory disease is not documented but it has been asserted that the mechanisms of secretory disease and galactopoiesis are closely related.
[[Image:Breast.png|thumb|center|Cross-section of the breast - By Original author: Patrick J. Lynch. Reworked by Morgoth666 to add numbered legend arrows. - Patrick J. Lynch, medical illustrator, CC BY 3.0, https://commons.wikimedia.org/w/index.php?curid=2676813]]


Permeability of the alveolar and ductal [[epithelia]] is mostly controlled by tight junction regulation and is closely linked to galactopoiesis and possibly secretory disease. The tight junctions are regulated by a multitude of systemic (prolactin, [[progesterone]], [[glucocorticoid]]s) and local (intramammary pressure, [[TGF-beta]], [[osmotic]] balance) factors.
1) Chest wall <br>2) Pectoralis muscles <br>3) Lobules <br>4) Nipple <br>5) Areola <br>6) Milk duct <br>7) Fatty tissue <br>8) Skin


Current smokers have the worst [[prognosis]] and highest rate of recurrent [[abscess]]es.


[[Acromegaly]] may present with symptoms of non-puerperal mastitis.


'''Surface anatomy of the breast'''




[[Image:Breast1.jpg|thumb|center|Surface anatomy of the breast - By Original: Ralf RoletschekDerivative: علاء نجار - Derivative from this file, CC BY-SA 3.0, https://commons.wikimedia.org/w/index.php?curid=46044299]]


===Terminology===
===Pathogenesis===
Depending on appearance, symptoms, aetiological assumptions and histopathological findings a variety of terms has been used to describe mastitis and various related aspects.
====Non-puerperal Mastitis====


* '''Galactopoiesis:''' milk production
Most clinically significant cases of non-puerperal mastitis start as [[inflammation]] of the ductal and [[lobular]] system and possibly the immediate surrounding [[tissue]]. 


* '''Secretory disease:''' aberrant secretory activity in the lobular and lactiferous duct system, believed to be the most frequent factor causing galactophoritis. The secretions may be milk like or apocrine luminal fluid.
Development of non-puerperal mastitis is the result of secretory [[stasis]] in about 80% of cases.  The retained [[secretions]] can get infected or lead to [[inflammation]] by causing mechanical [[injury]] leading to leakage of the [[lactiferous duct|lactiferous ducts]].  [[Autoimmune]] reaction to the [[secretion|secretions]] may also be a factor.


* '''Retention syndrome (aka retention mastitis):''' accumulation of secretions in the ducts with mainly intraductal inflammation.


* '''Galactostasis:''' like retention syndrome where the secret is known to be milk.
====Puerperal Mastitis====


* '''Galactophoritis:''' inflammation of the lobular and lactiferous duct system, mainly resulting from secretory disease and retention syndrome.
Development of puerperal mastitis occurs when [[bacteria]], often from patients [[skin]] or the baby's [[mouth]]/[[nostrils]],<ref>{{cite journal | title=A case-control study of mastitis: nasal carriage of ''Staphylococcus aureus'' | author=Amir LH, Garland SM, Lumley J. | journal=BMC Family Practice. | year=2006 | volume=7 | pages=57 | doi=10.1186/1471-2296-7-57 }}</ref> enters a [[milk]] [[duct]] through a crack in the [[nipple]].  


* '''Plasma cell mastitis:''' plasma cells from the intraductal inflammation infiltrate surrounding tissue.
Several mechanisms, listed below, are thought to lead to the pathogenesis of mastitis:  
* Secretory disease or [[galactorrhea]]
* Changes in [[permeability]] of [[lactiferous duct]]s (retention syndrome)
* Blockage of [[lactiferous duct]]s, for example duct plugging caused by [[squamous metaplasia]] of [[lactiferous duct]]s
* [[Trauma]] or [[injury]]
* Mechanical irritation caused by [[retention syndrome]] or [[Fibrocystic Disease|fibrocystic]] condition
* [[Infection]]
* [[Autoimmune]] reaction to [[luminal]] [[fluid]]


* '''Duct ectasia:''' literally widening of lactiferous ducts - relatively common finding in breast exams, increase with age. Strongly correlated with cyclic and very strongly with noncyclic breast pain. Correlation with mastitis is of anecdotal quality and has been questioned by recent research.
Approximately a quarter of patients may be [[hyperprolactinemia|hyperprolactinemic]].  There has been a strong association with [[fibrocystic breast disease|fibrocystic condition]] and [[thyroid]] conditions. Up to 50% of patients may experience transient [[hyperprolactinemia]] possibly caused by [[inflammation]] or treatment and a significant number of patients may have abnormally high [[prolactin]] reserve.<ref name="pmid2918655">{{cite journal| author=Peters F, Schuth W| title=Hyperprolactinemia and nonpuerperal mastitis (duct ectasia). | journal=JAMA | year= 1989 | volume= 261 | issue= 11 | pages= 1618-20 | pmid=2918655 | doi= | pmc= | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=2918655}}</ref><ref name="pmid26179543">{{cite journal| author=Kutsuna S, Mezaki K, Nagamatsu M, Kunimatsu J, Yamamoto K, Fujiya Y et al.| title=Two Cases of Granulomatous Mastitis Caused by Corynebacterium kroppenstedtii Infection in Nulliparous Young Women with Hyperprolactinemia. | journal=Intern Med | year= 2015 | volume= 54 | issue= 14 | pages= 1815-8 | pmid=26179543 | doi=10.2169/internalmedicine.54.4254 | pmc= | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=26179543}}</ref>


* '''Duct ectasia syndrome:''' in older literature this was used as synonym for nonpuerperal mastitis with recurring breast abscess, nipple discharge and possibly associated fibrocystic condition with blue dome cysts. Recent research shows that duct ectasia is only very weakly correlated with mastitis symptomes (inflammation, breast abscess). The use of the terms Duct Ectasia and Duct Ectasia Syndrome is inconsistent throughout the literature.
[[TSH]], [[prolactin]], and [[IGF-1]] are important systemic factors in [[galactopoiesis]]. The significance of these factors in secretory [[disease]] is not well documented but it has been asserted that the mechanisms of secretory disease and [[galactopoiesis]] are closely related.


* '''Squamous metaplasia of lactiferous ducts:''' cuboid cells in the epithelial lining of the lactiferous ducts transform ([[squamous metaplasia]]) to squamous epithelial cells. Present in many cases of subareolar abscesses.
[[Alveolar]] and ductal [[epithelia]] [[permeability]] is mostly controlled by [[tight junction]] regulation and is closely linked to [[galactopoiesis]] and secretory disease.  The [[tight junctions]] are regulated by a multitude of systemic ([[prolactin]], [[progesterone]], [[glucocorticoid]]s) and local (intramammary pressure, [[TGF-beta]], [[osmotic]] balance) factors.


* '''Subareolar abscess:''' [[abscess]] bellow or in close vicinity of the [[areola]]. Mostly resulting from galactophoritis.
[[Acromegaly]] may present with symptoms of non-puerperal mastitis.


* '''Retroareolar abscess:''' deeper (closer to chest) than the lobular ductal  system and thus deeper than a subareolar abscess.
===Microscopic pathology===


* '''Periductal inflammation (aka periductal mastitis):''' inflammation infiltrated tissue surrounding lactiferous ducts. Almost synonym for subaerolar abscess. May be just a different name for plasma cell mastitis.
[[Histopathology]] of [[granulomatous]] mastitis shows characteristic distribution of [[granulomatous]] [[inflammation]] which remains the gold standard for diagnosis.<ref name="pmid20030652">{{cite journal| author=Ocal K, Dag A, Turkmenoglu O, Kara T, Seyit H, Konca K| title=Granulomatous mastitis: clinical, pathological features, and management. | journal=Breast J | year= 2010 | volume= 16 | issue= 2 | pages= 176-82 | pmid=20030652 | doi=10.1111/j.1524-4741.2009.00879.x | pmc= | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=20030652}}</ref>


* '''Fistula:''' fine channel draining an abscess cavity
Histologically, [[lupus]] mastitis is seen as [[lymphocytic]] [[lobular]] [[panniculitis]] and [[hyaline]] [[sclerosis]] of the [[adipose tissue]]. This histologic finding is required to make an accurate diagnosis.<ref name="pmid19098467">{{cite journal| author=Summers TA, Lehman MB, Barner R, Royer MC| title=Lupus mastitis: a clinicopathologic review and addition of a case. | journal=Adv Anat Pathol | year= 2009 | volume= 16 | issue= 1 | pages= 56-61 | pmid=19098467 | doi=10.1097/PAP.0b013e3181915ff7 | pmc= | url=http://www.ncbi.nlm.nih.gov/entrez/eutils/elink.fcgi?dbfrom=pubmed&tool=sumsearch.org/cite&retmode=ref&cmd=prlinks&id=19098467}}</ref>
 
* '''Zuska's disease:''' periareolar abscess associated with squamous metaplasia of lactiferous ducts. Some authors also associate this with nipple discharge.


==References==
==References==
{{reflist|2}}
{{reflist|2}}
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Latest revision as of 22:39, 29 July 2020

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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Prince Tano Djan, BSc, MBChB [2]

Overview

Most clinically significant cases of non-puerperal mastitis start as inflammation of the ductal and lobular system and possibly the immediate surrounding tissue. Development of non-puerperal mastitis is the result of secretory stasis whereas puerperal mastitis occurs when bacteria, often from the patient's skin or the baby's mouth/nostrils,[1] enters a milk duct through a crack in the nipple.

Pathophysiology

Anatomy of the breast

The images below show a general overview of breast anatomy.

Cross-section of the breast - By Original author: Patrick J. Lynch. Reworked by Morgoth666 to add numbered legend arrows. - Patrick J. Lynch, medical illustrator, CC BY 3.0, https://commons.wikimedia.org/w/index.php?curid=2676813

1) Chest wall
2) Pectoralis muscles
3) Lobules
4) Nipple
5) Areola
6) Milk duct
7) Fatty tissue
8) Skin


Surface anatomy of the breast


Surface anatomy of the breast - By Original: Ralf RoletschekDerivative: علاء نجار - Derivative from this file, CC BY-SA 3.0, https://commons.wikimedia.org/w/index.php?curid=46044299

Pathogenesis

Non-puerperal Mastitis

Most clinically significant cases of non-puerperal mastitis start as inflammation of the ductal and lobular system and possibly the immediate surrounding tissue.

Development of non-puerperal mastitis is the result of secretory stasis in about 80% of cases. The retained secretions can get infected or lead to inflammation by causing mechanical injury leading to leakage of the lactiferous ducts. Autoimmune reaction to the secretions may also be a factor.


Puerperal Mastitis

Development of puerperal mastitis occurs when bacteria, often from patients skin or the baby's mouth/nostrils,[2] enters a milk duct through a crack in the nipple.

Several mechanisms, listed below, are thought to lead to the pathogenesis of mastitis:

Approximately a quarter of patients may be hyperprolactinemic. There has been a strong association with fibrocystic condition and thyroid conditions. Up to 50% of patients may experience transient hyperprolactinemia possibly caused by inflammation or treatment and a significant number of patients may have abnormally high prolactin reserve.[3][4]

TSH, prolactin, and IGF-1 are important systemic factors in galactopoiesis. The significance of these factors in secretory disease is not well documented but it has been asserted that the mechanisms of secretory disease and galactopoiesis are closely related.

Alveolar and ductal epithelia permeability is mostly controlled by tight junction regulation and is closely linked to galactopoiesis and secretory disease. The tight junctions are regulated by a multitude of systemic (prolactin, progesterone, glucocorticoids) and local (intramammary pressure, TGF-beta, osmotic balance) factors.

Acromegaly may present with symptoms of non-puerperal mastitis.

Microscopic pathology

Histopathology of granulomatous mastitis shows characteristic distribution of granulomatous inflammation which remains the gold standard for diagnosis.[5]

Histologically, lupus mastitis is seen as lymphocytic lobular panniculitis and hyaline sclerosis of the adipose tissue. This histologic finding is required to make an accurate diagnosis.[6]

References

  1. Amir LH, Garland SM, Lumley J. (2006). "A case-control study of mastitis: nasal carriage of Staphylococcus aureus". BMC Family Practice. 7: 57. doi:10.1186/1471-2296-7-57.
  2. Amir LH, Garland SM, Lumley J. (2006). "A case-control study of mastitis: nasal carriage of Staphylococcus aureus". BMC Family Practice. 7: 57. doi:10.1186/1471-2296-7-57.
  3. Peters F, Schuth W (1989). "Hyperprolactinemia and nonpuerperal mastitis (duct ectasia)". JAMA. 261 (11): 1618–20. PMID 2918655.
  4. Kutsuna S, Mezaki K, Nagamatsu M, Kunimatsu J, Yamamoto K, Fujiya Y; et al. (2015). "Two Cases of Granulomatous Mastitis Caused by Corynebacterium kroppenstedtii Infection in Nulliparous Young Women with Hyperprolactinemia". Intern Med. 54 (14): 1815–8. doi:10.2169/internalmedicine.54.4254. PMID 26179543.
  5. Ocal K, Dag A, Turkmenoglu O, Kara T, Seyit H, Konca K (2010). "Granulomatous mastitis: clinical, pathological features, and management". Breast J. 16 (2): 176–82. doi:10.1111/j.1524-4741.2009.00879.x. PMID 20030652.
  6. Summers TA, Lehman MB, Barner R, Royer MC (2009). "Lupus mastitis: a clinicopathologic review and addition of a case". Adv Anat Pathol. 16 (1): 56–61. doi:10.1097/PAP.0b013e3181915ff7. PMID 19098467.

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