Expression of Podocyte-Associated Molecules in Acquired Human Kidney Diseases

Koop, Klaas; Eikmans, Michael; Baelde, Hans J.; Kawachi, Hiroshi; Heer, Emile de; Paul, Leendert C.; Bruijn, Jan A.

doi:10.1097/01.asn.0000078803.53165.c9

Cited by 264 publications

(224 citation statements)

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“…Mutations in such genes often do not cause early embryonic lethality but rather manifest disease at the time when the function of these genes becomes critical for a specific tissue and subsequently for organismal survival (D'Agati 2008). In acquired disease like diabetes or hypertension, the vulnerability of a specific organ to the systemic disease is defined by the expression of tissue-specific genes (Doublier et al 2003;Koop et al 2003;Woroniecka et al 2011). Defining cell-lineage-specific transcripts therefore has immediate clinical implications for such cell lineages.…”

Section: Discussionmentioning

confidence: 99%

Defining cell-type specificity at the transcriptional level in human disease

et al. 2013

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Cell-lineage–specific transcripts are essential for differentiated tissue function, implicated in hereditary organ failure, and mediate acquired chronic diseases. However, experimental identification of cell-lineage–specific genes in a genome-scale manner is infeasible for most solid human tissues. We developed the first genome-scale method to identify genes with cell-lineage–specific expression, even in lineages not separable by experimental microdissection. Our machine-learning–based approach leverages high-throughput data from tissue homogenates in a novel iterative statistical framework. We applied this method to chronic kidney disease and identified transcripts specific to podocytes, key cells in the glomerular filter responsible for hereditary and most acquired glomerular kidney disease. In a systematic evaluation of our predictions by immunohistochemistry, our in silico approach was significantly more accurate (65% accuracy in human) than predictions based on direct measurement of in vivo fluorescence-tagged murine podocytes (23%). Our method identified genes implicated as causal in hereditary glomerular disease and involved in molecular pathways of acquired and chronic renal diseases. Furthermore, based on expression analysis of human kidney disease biopsies, we demonstrated that expression of the podocyte genes identified by our approach is significantly related to the degree of renal impairment in patients. Our approach is broadly applicable to define lineage specificity in both cell physiology and human disease contexts. We provide a user-friendly website that enables researchers to apply this method to any cell-lineage or tissue of interest. Identified cell-lineage–specific transcripts are expected to play essential tissue-specific roles in organogenesis and disease and can provide starting points for the development of organ-specific diagnostics and therapies.

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Section: Discussionmentioning

confidence: 99%

Defining cell-type specificity at the transcriptional level in human disease

et al. 2013

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“…From an etiological standpoint, FSGS may be associated with a variety of conditions, including viral infections (human immunodeficiency virus [HIV], simian virus 40 [SV40] , parvovirus B19), several drugs (heroin, pamidronate, interferon), adaptive to hyperfiltration (as in hypertension, obesity, and sickle-cell anemia), and genetic disorders (familiar forms), and may be idiopathic (11) . Podocyte injury is the core pathophysiological event of FSGS and some studies have found anomalous expression of podocyte proteins in FSGS (2,10,16) Table and Figure). Studies of these variants demonstrated correlation with distinct clinical characteristics and prognostic and therapeutic implications (4,18) .…”

Section: Introductionmentioning

confidence: 99%

Study of the morphologic variants of focal segmental glomerulosclerosis: a Brazilian report

Testagrossa¹,

Malheiros²

2012

J. Bras. Patol. Med. Lab.

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“…These genomic studies lead to the determination of a molecular topology for SD, required for maintaining the homeostasis of podocytespodocytes [21]. Notably, the decreases of SD-related molecules (such as podocin and CD2AP) are observed in many types of CKD, regardless of the primary etiology [1,19].…”

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confidence: 99%

Decreases in Podocin, CD2-Associated Protein (CD2AP) and Tensin2 May Be Involved in Albuminuria during Septic Acute Renal Failure

Kato

Mizuno-Horikawa

Mizuno

2011

The Journal of Veterinary Medical Science

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ABSTRACT. Podocytes have a peculiar structure constituting slit diaphragm (SD) and foot process (FP), and play essential roles in the glomerular filtration barrier. There is now ample evidence that SD-and FP-associated molecules, such as podocin and CD2-associated protein (CD2AP), are down-regulated during albuminuria of chronic kidney disease. However, it is still unclear whether these molecules are altered during acute renal failure (ARF) with albuminuria. Using lipopolysaccharide (LPS)-treated mice as a model of septic ARF, we provide evidence that the expression of SD-and FP-associated molecules becomes faint, along with albuminuria. In the LPS-treated mice, urinary albumin levels gradually increased, associated with the elevation of blood urea nitrogen levels, indicating the successful induction of albuminuria during septic ARF. In this pathological process, glomerular podocin expression became faint, especially at 36 hr post-LPS challenge (i.e., a peak of albuminuria). Likewise, LPS treatment led to a significant decrease in CD2AP, an anchorage between podocin and F-actin. With regard to this, tensin2 is a novel molecule that stabilizes F-actin extension. Interestingly, glomerular tensin2 expression levels were also decreased during the albuminuric phase, associated with losses of glomerular F-actin and synaptopodin under septic states. As a result, there were some lesions of podocytic FP effacement, as shown by electron microscopy. Based on these data, we emphasize the importance of concomitant decreases in podocin, CD2AP and tensin2 during septic ARF-associated proteinuria.

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Expression of Podocyte-Associated Molecules in Acquired Human Kidney Diseases

Cited by 264 publications

References 50 publications

Defining cell-type specificity at the transcriptional level in human disease

Defining cell-type specificity at the transcriptional level in human disease

Study of the morphologic variants of focal segmental glomerulosclerosis: a Brazilian report

Decreases in Podocin, CD2-Associated Protein (CD2AP) and Tensin2 May Be Involved in Albuminuria during Septic Acute Renal Failure

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