Identification of the Tuberous Sclerosis Gene
            <i>TSC1</i>
            on Chromosome 9q34

Slegtenhorst, Marjon van; Hoogt, Ronald de; Hermans, C. J.; Nellist, Mark; Janssen, Bart; Verhoef, Senno; Lindhout, Dick; Ouweland, Ans van den; Halley, Dicky; Young, Janet M.; Burley, Mari-Wyn; Jeremiah, Steve; Woodward, Karen; Nahmias, Joseph; Fox, Margaret; Ekong, Rosemary; Osborne, J. P.; Wolfe, Jonathan; Povey, Sue; Snell, Russell G.; Cheadle, Jeremy P.; Jones, A. R.; Tachataki, Maria; Ravine, David; Sampson, Julian R.; Reeve, Mary Pat; Richardson, Paul M.; Wilmer, Friederike; Munro, Cheryl; Hawkins, Trevor; Sepp, Tiina; Ali, Johari Bin Mohd; Ward, Susannah; Green, Andrew J.; Yates, John R.; Kwiatkowska, J.; Henske, Elizabeth P.; Short, M. Priscilla; Haines, Jonathan; Jóźwiak, Sergiusz; Kwiatkowski, David J.

doi:10.1126/science.277.5327.805

Cited by 1,518 publications

(809 citation statements)

References 43 publications

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“…TSC1 and TSC2 are widely expressed in human tissues, such as heart, brain, lung, liver, kidney, pancreas and skeletal muscle (Consortium, 1993;van Slegtenhorst et al, 1997;Huang and Manning, 2008). The two proteins interact through coiled-coil domains to form a stable, functional heterodimer (van Slegtenhorst et al, 1998).…”

Section: Regulation Of the Tsc1:tsc2 Complexmentioning

confidence: 99%

“…Loss of chromosome 16p (locus for TSC2) or promoter hypermethylation of the TSC genes has been detected in a substantial proportion of ovarian, gall bladder and breast cancer (Knowles et al, 2003;Jiang et al, 2005). Germ-line mutations in TSC1 and TSC2 predispose to TSC (Consortium, 1993;van Slegtenhorst et al, 1997), which is characterized by the development of widespread hamartomas in several organs including brain (cortical tubers and subependymal glial nodules), kidneys (angiomyolipomas, AML), skin ((angio) fibromas), heart (rhabdomyomas) and lungs (lymphangioleiomyomatosis (LAM)) ( Table 1). In addition, these patients develop early onset brain cancer (subependymal giant cell astrocytomas (SEGAs)) and different types of renal cancer (Table 1) (Schwartz et al, 2007;Curatolo et al, 2008;Ess, 2010).…”

Section: Nf1mentioning

confidence: 99%

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The long and winding road to rational treatment of cancer associated with LKB1/AMPK/TSC/mTORC1 signaling

et al. 2011

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The liver kinase B1 (LKB1)/adenosine mono-phosphateactivated protein kinase (AMPK)/tuberous sclerosis complex (TSC)/mammalian target of rapamycin (mTOR) complex (mTORC1) cassette constitutes a canonical signaling pathway that integrates information on the metabolic and nutrient status and translates this into regulation of cell growth. Alterations in this pathway are associated with a wide variety of cancers and hereditary hamartoma syndromes, diseases in which hyperactivation of mTORC1 has been described. Specific mTORC1 inhibitors have been developed for clinical use, and these drugs have been anticipated to provide efficient treatment for these diseases. In the present review, we provide an overview of the metabolic LKB1/AMPK/TSC/mTORC1 pathway, describe how its aberrant signaling associates with cancer development, and indicate the difficulties encountered when biochemical data are extrapolated to provide avenues for rational treatment of disease when targeting this signaling pathway. A careful examination of preclinical and clinical studies performed with rapamycin or derivatives thereof shows that although results are encouraging, we are only half way in the long and winding road to design rationale treatment targeted at the LKB1/ AMPK/TSC/mTORC1 pathway. Inherited cancer syndromes associated with this pathway such as the PeutzJeghers syndrome and TSC, provide perfect models to study the relationship between genetics and disease phenotype, and to delineate the complexities that underlie translation of biochemical and genetical information to clinical management, and thus provide important clues for devising novel rational medicine for cancerous diseases in general.

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Section: Regulation Of the Tsc1:tsc2 Complexmentioning

confidence: 99%

Section: Nf1mentioning

confidence: 99%

The long and winding road to rational treatment of cancer associated with LKB1/AMPK/TSC/mTORC1 signaling

et al. 2011

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“…TSC and LAM result from the inactivation of either of the two tumor-suppressor genes, TSC1 that encodes hamartin (TSC1), and TSC2 that encodes tuberin (TSC2) (van Slegtenhorst et al, 1997;Carsillo et al, 2000;Sato et al, 2002). TSC1 and TSC2 form an active complex (TSC1/2) that negatively regulates mammalian target of rapamycin complex 1 (mTORC1) signaling, which promotes cell growth (Huang and Manning, 2008).…”

Section: Introductionmentioning

confidence: 99%

Rheb activates AMPK and reduces p27Kip1 levels in Tsc2-null cells via mTORC1-independent mechanisms: implications for cell proliferation and tumorigenesis

et al. 2010

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“…The term CHARGE is an acronym for the syndrome's six core features: C, coloboma of the iris/retina; H, heart defects; A, atresia of the choanae; R, retardation of growth/development; G, genital abnormalities; and E, ear abnormalities. Occurring once in every 8500-10,000 live births [42,43], CHARGE syndrome also involves a range of secondary features, including deafness, laryngomalacia, vestibulocochlear defects, facial [80][81][82][83][84][85][86][87] CHARGE = C, coloboma of the iris/retina; H, heart defects; A, atresia of the choanae; R, retardation of growth/development; G, genital abnormalities; and E, ear abnormalities; PI3K = phosphoinositide 3-kinase; AKT = protein kinase B; MAPK = mitogen-activated protein kinase; mTOR = mammalian target of rapamycin nerve palsy, and oral clefts [44][45][46][47]. Many individuals with CHARGE syndrome are reported to exhibit autistic-like behaviors, with an estimated 27.5% meeting classification for autism [45].…”

Section: Charge Syndromementioning

confidence: 99%

“…These tumors, known as hamartomas, have an unpredictable distribution, but are often found within the brain, the skin, the heart, the kidneys, and the lungs [80,81]. TSC is associated with a variety of cognitive and developmental deficits, including ID, ADHD, and epilepsy.…”

Section: Tuberous Sclerosis Complexmentioning

confidence: 99%

Discovery of Rare Mutations in Autism: Elucidating Neurodevelopmental Mechanisms

et al. 2015

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Autism spectrum disorder (ASD) is a group of highly genetic neurodevelopmental disorders characterized by language, social, cognitive, and behavioral abnormalities. ASD is a complex disorder with a heterogeneous etiology. The genetic architecture of autism is such that a variety of different rare mutations have been discovered, including rare monogenic conditions that involve autistic symptoms. Also, de novo copy number variants and single nucleotide variants contribute to disease susceptibility. Finally, autosomal recessive loci are contributing to our understanding of inherited factors. We will review the progress that the field has made in the discovery of these rare genetic variants in autism. We argue that mutation discovery of this sort offers an important opportunity to identify neurodevelopmental mechanisms in disease. The hope is that these mechanisms will show some degree of convergence that may be amenable to treatment intervention.

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Identification of the Tuberous Sclerosis Gene TSC1 on Chromosome 9q34

Cited by 1,518 publications

References 43 publications

The long and winding road to rational treatment of cancer associated with LKB1/AMPK/TSC/mTORC1 signaling

The long and winding road to rational treatment of cancer associated with LKB1/AMPK/TSC/mTORC1 signaling

Rheb activates AMPK and reduces p27Kip1 levels in Tsc2-null cells via mTORC1-independent mechanisms: implications for cell proliferation and tumorigenesis

Discovery of Rare Mutations in Autism: Elucidating Neurodevelopmental Mechanisms

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