Peripheral Myelin Protein 22 Is in Complex with α6β4 Integrin, and Its Absence Alters the Schwann Cell Basal Lamina

Amici, Stephanie A.; Dunn, William A.; Murphy, Andrew J.; Adams, Niels C.; Gale, Nicholas W.; Valenzuela, David M.; Yancopouloš, George D.; Notterpek, Lucia

doi:10.1523/jneurosci.2618-05.2006

Cited by 63 publications

(87 citation statements)

References 71 publications

(88 reference statements)

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“…Table 1 lists representative genes for each area, plus annotation of which other treated populations these genes appear in (the complete list is available at http://www.rpi.edu/∼bennek/TissueEng/ln5.html). Area 1 (Ln-5 hMSC) was characterized by a number of genes encoding signaling proteins, many of which are associated with ECMstimulated pathways, cell survival, and regulation of cell growth in non-osteoblast lineages (e.g., caldesmon [Hai et al, 2006]; calpain 2 [Westhoff et al, 2004]; beta4 associated protein [Amici et al, 2006]). Most of these genes (31 of 46) were found in Area 1 for hMSC stimulated by collagen I, vitronectin, or OS medium as well (e.g., Table 1, column 3).…”

Section: Resultsmentioning

confidence: 99%

Laminin-5 activates extracellular matrix production and osteogenic gene focusing in human mesenchymal stem cells

et al. 2007

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We recently reported that laminin-5, expressed by human mesenchymal stem cells (hMSC), stimulates osteogenic gene expression in these cells in the absence of any other osteogenic stimulus. Here we employ two dimensional liquid chromatography and tandem mass spectrometry, along with the Database for Annotation, Visualization and Integrated Discovery (DAVID), to obtain a more comprehensive profile of the protein (and hence gene) expression changes occurring during laminin-5-induced osteogenesis of hMSC. Specifically, we compare the protein expression profiles of undifferentiated hMSC, hMSC cultured on laminin-5 (Ln-5 hMSC), and fully differentiated human osteoblasts (hOST) with profiles from hMSC treated with well-established osteogenic stimuli (collagen I, vitronectin, or dexamethazone). We find a marked reduction in the number of proteins (e.g., those involved with calcium signaling and cellular metabolism) expressed in Ln-5 hMSC compared to hMSC, consistent with our previous finding that hOST express far fewer proteins than do their hMSC progenitors, a pattern we call "osteogenic gene focusing." This focused set, which resembles an intermediate stage between hMSC and mature hOST, mirrors the expression profiles of hMSC exposed to established osteogenic stimuli and includes osteogenic extracellular matrix proteins (collagen, vitronectin) and their integrin receptors, calcium signaling proteins, and enzymes involved in lipid metabolism. These results provide direct evidence that laminin-5 alone stimulates global changes in gene/protein expression in hMSC that lead to commitment of these cells to the osteogenic phenotype, and that this commitment correlates with extracellular matrix production.

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Section: Resultsmentioning

confidence: 99%

Laminin-5 activates extracellular matrix production and osteogenic gene focusing in human mesenchymal stem cells

et al. 2007

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“…β4 integrin interacts with Pmp22, but mutant mice have different severity of phenotypes β4 integrin has recently been shown to form a complex with Pmp22 (Amici et al, 2006). Heterozygous loss-of-function mutations in PMP22 in mice and men cause a milder tomacular neuropathy, evident only after compression (Hereditary Neuropathy with liability to Pressure Palsy (HNPP).…”

Section: Absence Of α6β4 Integrin In Schwann Cells Does Not Affect Scmentioning

confidence: 99%

“…Heterozygous loss-of-function mutations in PMP22 in mice and men cause a milder tomacular neuropathy, evident only after compression (Hereditary Neuropathy with liability to Pressure Palsy (HNPP). Heterozygous null mice for Pmp22 resemble HNPP pathology (Adlkofer et al, 1995), whereas homozygous null mice have a severe dys-and de-myelinating neuropathy with both hypomyelination and tomacula (Adlkofer et al, 1995;Amici et al, 2006). In these mice, an impaired organization of the basal lamina and a drastic reduction in the levels of β4 integrin was reported, suggesting a role for Pmp22 in stabilizing laminin-integrin interactions (Amici et al, 2006).…”

Section: Absence Of α6β4 Integrin In Schwann Cells Does Not Affect Scmentioning

confidence: 99%

“…Heterozygous null mice for Pmp22 resemble HNPP pathology (Adlkofer et al, 1995), whereas homozygous null mice have a severe dys-and de-myelinating neuropathy with both hypomyelination and tomacula (Adlkofer et al, 1995;Amici et al, 2006). In these mice, an impaired organization of the basal lamina and a drastic reduction in the levels of β4 integrin was reported, suggesting a role for Pmp22 in stabilizing laminin-integrin interactions (Amici et al, 2006). A hypothesis arising from this observation is that laminin-integrin interactions at the basal lamina contribute to the stability of the myelin sheath.…”

Section: Absence Of α6β4 Integrin In Schwann Cells Does Not Affect Scmentioning

confidence: 99%

“…Fourth, α6β4 integrin in epithelia amplifies neuregulin signaling (Guo et al, 2006), which is crucial at multiple stages of Schwann cell development (reviewed in (Nave and Salzer, 2006). Finally α6β4 integrin interacts with PMP-22, a myelin protein mutated in Charcot-Marie-Tooth 1A neuropathy (Amici et al, 2006). Against a role for α6β4 integrin, myelination starts normally in newborn nerves and dorsal root ganglia explants from mice dying at post-natal day 1 (P1) due to β4 inactivation (Frei et al, 1999).…”

Section: Introductionmentioning

confidence: 99%

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6 4 Integrin and Dystroglycan Cooperate to Stabilize the Myelin Sheath

Nodari¹,

Previtali²,

Dati³

et al. 2008

Journal of Neuroscience

103

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Schwann cells integrate signals deriving from the axon and the basal lamina to myelinate peripheral nerves. Integrin α6β4 is a laminin receptor synthesized by Schwann cells and displayed apposed to the basal lamina. α6β4 integrin expression in Schwann cells is induced by axons at the onset of myelination, and rise in adulthood. The β4 chain has a uniquely long cytoplasmic domain that interacts with intermediate filaments such as dystonin, important in peripheral myelination. Furthermore, α6β4 integrin binds peripheral myelin protein 22, whose alteration causes the most common demyelinating hereditary neuropathy. All these data suggest a role for α6β4 integrin in peripheral nerve myelination. Here we show that ablating α6β4 integrin specifically in Schwann cells of transgenic mice does not affect peripheral nerve development, myelin formation, maturation or regeneration. However, consistent with maximal expression in adult nerves, α6β4 integrin-null myelin is more prone to abnormal folding with aging. When the laminin receptor dystroglycan is also ablated, major folding abnormalities occur, associated with acute demyelination in some peripheral nervous system districts. These data indicate that, similar to its role in skin, α6β4 integrin confers stability to myelin in peripheral nerves.

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