Focal segmental glomerulosclerosis

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Focal segmental glomerulosclerosis Classification and external resources
ICD-10	N 00.-N 08. (with .1 suffix)
ICD-9	581.1
OMIM	603278 603965 607832
MedlinePlus	000478
eMedicine	med/2944
MeSH	D005923

Focal segmental glomerulosclerosis (FSGS) is a cause of nephrotic syndrome in children and adolescents, as well as an important cause of kidney failure in adults.^[1]

It is also known as "focal glomerular sclerosis".^[2]

It accounts for about a sixth of the cases of nephrotic syndrome.^[3] (Minimal change disease (MCD) is by far the most common cause of nephrotic syndrome in children: MCD and primary FSGS may have a similar cause.^[1])

1 Appearance
2 Classification
- 2.1 Pathologic variants
3 Causes
4 Diagnosis
5 Treatment
6 References
7 External links

[edit] Appearance

The individual components of the name refer to the appearance of the kidney tissue on biopsy: focal - only some of the glomeruli are involved (as opposed to diffuse), segmental - only part of an entire glomerulus is involved (as opposed to global),^[4] glomerulosclerosis - refers to scarring of the glomerulus (a part of the nephron (the functional unit of the kidney))

[edit] Classification

Depending on the cause it is broadly classified as

Primary, when no underlying cause is found; usually presents as nephrotic syndrome
Secondary, when an underlying cause is identified; usually presents with kidney failure and proteinuria. This is actually a heterogeneous group including numerous causes such as
- Infections such as HIV (known as HIV-Associated Nephropathy)
- Toxins and drugs such as heroin and pamidronate
- Familial forms
- Secondary to nephron loss and hyperfiltration, such as with chronic pyelonephritis and reflux, morbid obesity, diabetes mellitus

There are many other classification schemes also.

[edit] Pathologic variants

Five mutually exclusive variants of focal segmental glomerulosclerosis may be distinguished by the pathologic findings seen on renal biopsy:^[5]

Collapsing variant
Glomerular tip lesion variant
Cellular variant
Perihilar variant
Not otherwise specified (NOS) variant.

Recognition of these variants may have prognostic value in individuals with primary focal segmental glomerulosclerosis (i.e. where no underlying cause is identified). The collapsing variant is associated with higher rate of progression to end-stage renal disease, whereas glomerular tip lesion variant has low rate of progression to end-stage renal disease in most patients.^[5] Cellular variant shows similar clinical presentation to collapsing and glomerular tip variant but has intermediate outcomes between these two variants. However, because collapsing and glomerular tip variant show overlapping pathologic features with cellular variant, this intermediate difference in clinical outcomes may reflect sampling bias in cases of cellular focal segmental glomerulosclerosis (i.e. unsampled collapsing variant or glomerular tip variant). The prognostic significance of perihilar and NOS variants has not yet been determined. The NOS variant is the most common subtype.^[5]

[edit] Causes

There are currently several known genetic causes of the hereditary forms of FSGS.

Gene	OMIM	Description
FSGS1: ACTN4	603278	The first gene involved with this disorder is ACTN4, which encodes alpha-actinin 4. This protein crosslinks bundles of actin filaments and is present in the podocyte. Mutations in this protein associated with FSGS result in increased affinity for actin binding, formation of intracellular aggregates, and decreased protein half-life. While it is unclear how these effects might lead to FSGS there are a number of theories. Firstly, protein aggregation may have a toxic effect on the podocyte. Secondly, decreased protein half-life or increased affinity for actin binding may alter actin polymerization and thereby affect the podocytes cytoskeletal architecture.^[6]
FSGS2: TRPC6	603965	A second gene associated with FSGS is TRPC6, which encodes a member of the canonical family of TRP channels. This family of ion channels conduct cations in a largely non-selective manner. As with ACTN4, TRPC6 is expressed in podocytes. While TRP channels can be activated through a variety of methods, TRPC6 is known to be activated by phospholipase C stimulation. There are at least 6 mutations in this channel, located throughout the channel. At least one of these mutations, P112Q, leads to increased intracellular calcium influx. It is unclear how this might lead to FSGS, though it has been proposed that it may result in alteration of podocyte dynamics or podocytopenia.^[6]
FSGS3: CD2AP	607832	Another gene that may be involved in hereditary forms of FSGS is the gene known as CD2AP (CD2 associated protein) or CMS (Cas binding protein with multiple SH3 domains). The protein expressed by this gene is expressed in podocytes where it interacts with fyn and synaptopodin. There is a report that a splicing mutation in this gene was found in two patients with HIV associated FSGS and this led to altered protein translation. This has been theorized to result in altered actin binding and, thus, alteration of the cytoskeletal podocyte architecture.^[6]
NPHS2	-	Mutations in the NPHS2 gene, which codes for the protein called podocin,^[7] can cause focal segmental glomerulosclerosis.^[8] This is a recessive form of FSGS.^{[citation needed]} An affected individual has two mutant copies of the NPHS2 gene, in contrast to ACTN4 and TRPC6 mediated forms of disease, which are dominant and require only one mutant copy of the gene. NPHS2-mediated FSGS is resistant to treatment with steroids.

[edit] Diagnosis

[edit] Symptoms and signs

In children and some adults, FSGS presents as a nephrotic syndrome (which is characterized by edema (associated with weight gain), hypoalbuminemia (low serum albumin (a protein) in the blood), hyperlipidemia and hypertension (high blood pressure)). In adults it may also present as kidney failure and proteinuria, without a full-blown nephrotic syndrome.

[edit] Tests

urinalysis
blood tests - cholesterol
kidney biopsy

[edit] Differential diagnosis

Minimal change disease, especially in children
several others

[edit] Treatment

Salt restriction and diuretics (water pills), such as furosemide, for edema
Antihypertensives (especially ACEIs) - if the blood pressure is too high
treat present hyperlipidemia (e.g. statins, fibrates)
Aldosterone antagonist to decrease proteinuria and thus offer a degree of reno-protection
Corticosteroids, such as prednisone - based on the clinical judgment of physician (no broad consensus/guideline)^{[citation needed]}
Cytotoxics, such as cyclophosphamide may be used to induce remission in patients presenting with FSGS refractory to corticosteroids, or in patients who do not tolerate steroids.
Plasmapheresis - blood cleansing using a machine to remove the patient's blood plasma and replacing it with donor plasma.
None - sometimes none of the above works and the patient will require dialysis with possibly later transplantation of a new kidney.^{[citation needed]}

[edit] References

^ ^a ^b Kumar V, Fausto N, Abbas A (editors) (2003). Robbins & Cotran Pathologic Basis of Disease (7th ed.), Saunders. pp.pp. 982-3. ISBN 978-0-721-60187-8.
^ focal segmental glomerulosclerosis at Dorland's Medical Dictionary
^ "Renal Pathology". Retrieved on 2008-11-25.
^ "Focal_segmental_glomerulosclerosis of the Kidney". Retrieved on 2008-11-25.
^ ^a ^b ^c Thomas DB, Franceschini N, Hogan SL, et al (2006). "Clinical and pathologic characteristics of focal segmental glomerulosclerosis pathologic variants". Kidney Int. 69 (5): 920–6. doi:10.1038/sj.ki.5000160. PMID 16518352.
^ ^a ^b ^c Mukerji N, Damodaran TV, Winn MP (2007). TRPC6 and FSGS: The latest TRP channelopathy. doi:10.1016/j.bbadis.2007.03.005. PMID 17459670.
^ Tsukaguchi H, Sudhakar A, Le TC, et al (December 2002). "NPHS2 mutations in late-onset focal segmental glomerulosclerosis: R229Q is a common disease-associated allele". J. Clin. Invest. 110 (11): 1659–66. doi:10.1172/JCI16242. PMID 12464671. PMC: 151634, http://dx.doi.org/10.1172/JCI16242.
^ Franceschini N, North KE, Kopp JB, McKenzie L, Winkler C (February 2006). "NPHS2 gene, nephrotic syndrome and focal segmental glomerulosclerosis: a HuGE review". Genet. Med. 8 (2): 63–75. doi:10.1097/01.gim.0000200947.09626.1c. PMID 16481888, http://meta.wkhealth.com/pt/pt-core/template-journal/lwwgateway/media/landingpage.htm?an=00125817-200602000-00001.

[edit] External links

NephCure Foundation Only organization solely committed to support research seeking the cause of Nephrotic Syndrome and FSGS, improve treatment and find the cure.
Kidcomm An online resource for parents dealing with childhood kidney diseases (FSGS, Nephrotic Syndrome and others)

v • d • e

Urinary system · Pathology · Urologic disease / Uropathy (N00-N39, 580-599)

Abdominal

Nephropathy/
(nephritis+
nephrosis)

Glomerulopathy/
glomerulitis/
(glomerulonephritis+
glomerulonephrosis)

By appearance

Non-proliferative	.0 Minimal change · .1 Focal segmental · .2 Membranous

Proliferative	.3 Mesangial proliferative · .4 Endocapillary proliferative .5/.6 Membranoproliferative/mesangiocapillary · .7 Rapidly progressive/crescentic

By syndrome

Nephritic syndrome · Nephrotic syndrome

By condition

IgA/Berger's · Diabetic · Post-streptococcal · Lupus · Amyloidosis

Tubulopathy/
tubulitis

Interstitium

Interstitial nephritis (Pyelonephritis, Danubian endemic familial nephropathy)

Any/all

General syndromes	Renal failure (Acute renal failure, Chronic renal failure)

Vascular	Renal artery stenosis · Hypertensive nephropathy · Renovascular hypertension

Other	Analgesic nephropathy · Renal osteodystrophy · Nephroptosis · Abderhalden-Kaufmann-Lignac syndrome

Ureter

Ureteritis · Ureterocele · Megaureter

Pelvic

Bladder	Cystitis (Interstitial cystitis, Trigonitis) · Neurogenic bladder · Vesicointestinal fistula · Vesicoureteral reflux

Urethra	Urethritis (Non-gonococcal urethritis) · Urethral syndrome · Urethral stricture

Any/all

Obstructive uropathy · Urinary tract infection · Retroperitoneal fibrosis · Urolithiasis (Kidney stone, Renal colic)

See also congenital, neoplasia, symptoms/signs

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