Homeotic Gene teashirt (tsh) Has a Neuroprotective Function in Amyloid-Beta 42 Mediated Neurodegeneration

Moran, Michael T; Tare, Meghana; Kango‐Singh, Madhuri; Singh, Amit

doi:10.1371/journal.pone.0080829

Cited by 21 publications

(35 citation statements)

References 78 publications

(135 reference statements)

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“…Drosophila has been a useful model organism for performing genetic screens to identify genes and pathways that modify phenotypes associated with neurodegenerative diseases, including spinocerebellar ataxia (Fernandez-Funez et al, 2000;Ren et al, 2011;Shieh and Bonini, 2011), Wolfram syndrome (Jones et al, 2014), Alzheimer’s disease (Moran et al, 2013;Shulman and Feany, 2003) and Huntington’s disease (Kazemi-Esfarjani and Benzer, 2000). Screens can be targeted, testing the effects of an array of known genes on a particular phenotype (Jones et al, 2014;Ren et al, 2011), or they can be unbiased, looking for any genes that modify a phenotype.…”

Section: 0 Drosophila Models Of Alsmentioning

confidence: 99%

“…Drosophila at any stage of development can be used, depending on the phenotype of interest (Batlevi et al, 2010;Rorth et al, 1998). Eye degeneration is a commonly used phenotypic output (Kazemi-Esfarjani and Benzer, 2000;Moran et al, 2013), although genetic screens have also been performed using survival (Li et al, 2014), wing posture (Shieh and Bonini, 2011), climbing (Shieh and Bonini, 2011) defects and axonal and synaptic degeneration (Wishart et al, 2012). Here we highlight the genes that have been identified as modifiers of TDP-43-associated neurodegeneration in Drosophila models of ALS.…”

Section: 0 Drosophila Models Of Alsmentioning

confidence: 99%

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A fruitful endeavor: Modeling ALS in the fruit fly

Casci

Pandey

2015

Brain Research

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For over a century Drosophila melanogaster, commonly known as the fruit fly, has been instrumental in genetics research and disease modeling. In more recent years, it has been a powerful tool for modeling and studying neurodegenerative diseases, including the devastating and fatal amyotrophic lateral sclerosis (ALS). The success of this model organism in ALS research comes from the availability of tools to manipulate gene/protein expression in a number of desired cell-types, and the subsequent recapitulation of cellular and molecular phenotypic features of the disease. Several Drosophila models have now been developed for studying the roles of ALS-associated genes in disease pathogenesis that allowed us to understand the molecular pathways that lead to motor neuron degeneration in ALS patients. Our primary goal in this review is to highlight the lessons we have learned using Drosophila models pertaining to ALS research.

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Section: 0 Drosophila Models Of Alsmentioning

confidence: 99%

Section: 0 Drosophila Models Of Alsmentioning

confidence: 99%

A fruitful endeavor: Modeling ALS in the fruit fly

Casci

Pandey

2015

Brain Research

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“…Several animal AD models have shown promise; however, our Drosophila model allows us to test other signaling pathways using genetic epistasis approaches (Pandey and Nichols, 2011;Lenz et al, 2013;Sabbagh et al, 2013;Sarkar et al, 2016;Deshpande et al, 2019). We previously reported the neuroprotective effects of the apical basal polarity gene crumbs (crb) (Moran et al, 2013;Steffensmeier et al, 2013) and the homeotic gene teashirt (tsh) (Moran et al, 2013) in Aβ42-mediated neurodegeneration. Interestingly, these genetic modifiers are members of the Hippo signaling pathway.…”

Section: Discussionmentioning

confidence: 99%

“…We previously reported the neuroprotective effects of the apical basal polarity gene crumbs (crb) (Moran et al, 2013;Steffensmeier et al, 2013) and the homeotic gene teashirt (tsh) (Moran et al, 2013), both members of the Hippo signaling pathway. However, the neuroprotective function of Hippo or JNK signaling interactions together has not been fully understood.…”

Section: Positive Feedback Loop Of Hippo and C-jun-amino-terminal Kinmentioning

confidence: 99%

“…As per the amyloid hypothesis, the accumulation of the Aβ42 peptides into plaques initiates a pathological cascade eventually leading to neurodegeneration (Tare et al, 2011;Selkoe and Hardy, 2016;Yeates et al, 2019). Since this hypothesis was postulated, several signaling pathways and genetic modifiers have been implicated in Aβ42-mediated neurodegeneration (Moran et al, 2013;Steffensmeier et al, 2013;Cutler et al, 2015;Yeates et al, 2019).…”

Section: Introductionmentioning

confidence: 99%

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A Positive Feedback Loop of Hippo- and c-Jun-Amino-Terminal Kinase Signaling Pathways Regulates Amyloid-Beta-Mediated Neurodegeneration

Irwin

Tare

Singh

et al. 2020

Front. Cell Dev. Biol.

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Alzheimer's disease (AD, OMIM: 104300) is an age-related disorder that affects millions of people. One of the underlying causes of AD is generation of hydrophobic amyloid-beta 42 (Aβ42) peptides that accumulate to form amyloid plaques. These plaques induce oxidative stress and aberrant signaling, which result in the death of neurons and other pathologies linked to neurodegeneration. We have developed a Drosophila eye model of AD by targeted misexpression of human Aβ42 in the differentiating retinal neurons, where an accumulation of Aβ42 triggers a characteristic neurodegenerative phenotype. In a forward deficiency screen to look for genetic modifiers, we identified a molecularly defined deficiency, which suppresses Aβ42-mediated neurodegeneration. This deficiency uncovers hippo (hpo) gene, a member of evolutionarily conserved Hippo signaling pathway that regulates growth. Activation of Hippo signaling causes cell death, whereas downregulation of Hippo signaling triggers cell proliferation. We found that Hippo signaling is activated in Aβ42-mediated neurodegeneration. Downregulation of Hippo signaling rescues the Aβ42-mediated neurodegeneration, whereas upregulation of Hippo signaling enhances the Aβ42-mediated neurodegeneration phenotypes. It is known that c-Jun-amino-terminal kinase (JNK) signaling pathway is upregulated in AD. We found that activation of JNK signaling enhances the Aβ42-mediated neurodegeneration, whereas downregulation of JNK signaling rescues the Aβ42-mediated neurodegeneration. We tested the nature of interactions between Hippo signaling and JNK signaling in Aβ42-mediated neurodegeneration using genetic epistasis approach. Our data suggest that Hippo signaling and JNK signaling, two independent signaling pathways, act synergistically upon accumulation of Aβ42 plaques to trigger cell death. Our studies demonstrate a novel role of Hippo signaling pathway in Aβ42-mediated neurodegeneration.

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Proximal fate marker homothorax marks the lateral extension of stalk‐eyed fly Cyrtodopsis whitei

Singh

Gogia

Chang

et al. 2019

Genesis

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The placement of eyes on insect head is an important evolutionary trait. The stalk-eyed fly, Cyrtodopsis whitei, exhibits a hypercephaly phenotype where compound eyes are located on lateral extension from the head while the antennal segments are placed inwardly on this stalk. This stalk-eyed phenotype is characteristic of the family Diopsidae in the Diptera order and dramatically deviates from other dipterans, such as Drosophila.Like other insects, the adult eye and antenna of stalk-eyed fly develop from a complex eye-antennal imaginal disc. We analyzed the markers involved in proximo-distal (PD) axis of the developing eye imaginal disc of the stalk-eyed flies. We used homothorax (hth) and distalless (dll), two highly conserved genes as the marker for proximal and distal fate, respectively. We found that lateral extensions between eye and antennal field of the stalk-eyed fly's eye-antennal imaginal disc exhibit robust Hth expression. Hth marks the head specific fate in the eye-and proximal fate in the antenna-disc. Thus, the proximal fate marker Hth expression evolves in the stalk-eyed flies to generate lateral extensions for the placement of the eye on the head. Moreover, during pupal eye metamorphosis, the lateral extension folds back on itself to place the antenna inside and the adult compound eye on the distal tip. Interestingly, the compound eye in other insects does not have a prominent PD axis as observed in the stalk-eyed fly. K E Y W O R D S dacshund, distalless, Drosophila, eye development, eye-antennal imaginal disc, homothorax, proximo-distal axis, stalk-eyed fly

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Homeotic Gene teashirt (tsh) Has a Neuroprotective Function in Amyloid-Beta 42 Mediated Neurodegeneration

Cited by 21 publications

References 78 publications

A fruitful endeavor: Modeling ALS in the fruit fly

A fruitful endeavor: Modeling ALS in the fruit fly

A Positive Feedback Loop of Hippo- and c-Jun-Amino-Terminal Kinase Signaling Pathways Regulates Amyloid-Beta-Mediated Neurodegeneration

Proximal fate marker homothorax marks the lateral extension of stalk‐eyed fly Cyrtodopsis whitei

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