Drp1 is widely, yet heterogeneously, distributed in the mouse central nervous system

Luo, Tingting; Dai, Chun-Qiu; Wang, Jiaqi; Wang, Zhengmei; Yang, Yi; Zhang, Kun-Long; Wu, Feifei; Yang, Yanling; Wang, Ya-Yun

doi:10.1186/s13041-020-00628-y

Cited by 11 publications

(8 citation statements)

References 52 publications

(68 reference statements)

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“…In mammalian cells, ssion/fusion events are mainly mediated by several large dynaminrelated GTPase proteins, including conserved dynamin-related GTPase (Drp1), conserved dynamin-related GTPase mitofusion 1 and 2 (Mfn1 and 2), and optic dominant atrophy 1 (Opa1). Our lab have published the data previously about the expression of Drp1 at high level on the soma of cerebellum Purkinje cells by the combination of immunohistochemistry and in situ hybridization on GAD67 (glutamic acid decarboxylase 67) -GFP (green uorescent protein) transgenic mice (Luo TT et al, 2020). The present ndings have con rmed the distribution pattern of Drp1 on Purkinje cells.…”

Section: Drp1/mfn1/mfn2supporting

confidence: 79%

Visualizing an convergence of three mitochondrial molecule mRNAs for DRP1/MFN2/UCP4 on soma of cerebellar Purkinje cells by RNAscope

Liu¹,

Luo²,

Wu³

et al. 2021

Preprint

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We know little about how mitochondrial dynamic are regulated in the Purkinje cells. To explore it, we first set up a transgenic mice in which Purkinje cells expressed tdTomato in the cerebellum of Gad2-cre;ZsGreen-tdTomatofl/fl mice. Secondly Double stainings verified tdTomato cells were Calbinin (CB)-positive Purkinje cells, but not colocalized either with astrocyte marker GFAP or with microglia marker Iba1. Thirdly, application of RNAscope in situ hybridization with the identification of mRNAs of mitochondrial fusion (Mfn2), calcium transporter (Mcu and Nclx) and uncoupling proteins (Ucp2 and Ucp4) were used onto Purkinje cells for specific spatial analysis. The RNAscope assay used a semi‑quantitative H scoring guideline to evaluate the staining results. The number of bins ranges from 0–4 according to the ACD scoring system. Moreover, ACD scoring system was used to calculate the overall H scores of Dendritic Weighted Formula (DWF) and Soma Weighted Formula (SWF). Our data for the first time demonstrated that Mfn2 mRNAs expression was evident in Prukinje cells with the H scores of DWF and SWF as 60 and 139, respectively. And few Ucp4 mRNAs expression was present in dendritic shafts of Prukinje cells with the H scores of DWF and SWF as 14 and 103, respectively. It should be noted that Mcu mRNAs, Nclx mRNAs, as well as Ucp2 mRNAs expression were only scattered on both soma and dendrites in Prukinje cells with the low H scores of DWF and SWF. Double RNAscope profiling of mitochondrial molecules showed The data showed Mfn1 mRNAs are present only in the soma of the Purkinje cells, instead of processes. Double RNAscope showed almost none of dots of Drp1 mRNAs was co-localized with dots of Mcu mRNAs, as well as almost none of dots of Ucp2 mRNAs was co-localized with dots of Mfn2 mRNAs. All of these results show the mitochondrial Drp1/Mfn2/UCP4 convergence on the Purkinje cells. Finally, a major focus of present research will be to develop new and more specific molecules that tune the activity of the Purkinje cells activate or inactivate and to address diseases for which such druglike molecules may open therapeutic windows for Purkinje cells-related manipulation in the clinic. The molecular identification of drug targets, mechanism of action, and structural basis of their activity will crucially enable preclinical development.

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Section: Drp1/mfn1/mfn2supporting

confidence: 79%

Visualizing an convergence of three mitochondrial molecule mRNAs for DRP1/MFN2/UCP4 on soma of cerebellar Purkinje cells by RNAscope

Liu¹,

Luo²,

Wu³

et al. 2021

Preprint

Self Cite

View full text Add to dashboard Cite

show abstract

“…In mammalian cells, ssion/fusion events are mainly mediated by several large dynaminrelated GTPase proteins, including conserved dynamin-related GTPase (Drp1), conserved dynamin-related GTPase mitofusion 1 and 2 (Mfn1 and 2), and optic dominant atrophy 1 (Opa1). Our lab have published the data previously about the expression of Drp1 at high level on the soma of cerebellum Purkinje cells by the combination of immunohistochemistry and in situ hybridization on GAD67 (glutamic acid decarboxylase 67) -GFP (green uorescent protein) transgenic mice [24]. The present ndings have con rmed the distribution pattern of Drp1 on Purkinje cells.…”

Section: Drp1/mfn1/mfn2supporting

confidence: 79%

“…According to our previous report [24], we demonstrated that Drp1 was overexpressed in the cerebellum Purkinje layer, while Drp1 and GAD67 also colabeled well in this area. Drp1 and GAD67 colabeling was lower in other nuclei.…”

Section: Drp1 (Green) and Mcu (Red)supporting

confidence: 65%

Visualizing a Convergence of Three Mitochondrial Molecule mRNAs for Drp1/Mfn2/Ucp4 on Soma of Cerebellar Purkinje Cells by RNAscope

Liu

Luo

et al. 2021

Preprint

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We know little about how mitochondrial dynamics regulates in the Purkinje cells. To explore it, we first set up the Gad2-cre:ZsGreen-tdTomatofl/fl mice where Purkinje cells expressed tdTomato in the cerebellum. Secondly, double stainings verified tdTomato cells were Calbinin (CB)-positive Purkinje cells, but colocalized neither with astrocyte marker GFAP nor with microglia marker Iba1. Thirdly, application of RNAscope in situ hybridization with the identification of mRNAs of mitofusin 2 (Mfn2), calcium transporter (Mcu and Nclx) and uncoupling proteins (Ucp2 and Ucp4) were used onto Purkinje cells for specific spatial analysis. Our findings demonstrated that Mfn2 mRNAs expression was evident in Purkinje cells. And few expressions of Ucp4 mRNAs were presented in dendritic shafts of Purkinje cells. It should be noted that Mcu, Nclx, and Ucp2 mRNAs expression were only scattered on both soma and dendrites in Purkinje cells. The double RNAscope profiling of mitochondrial molecules showed Mfn1 mRNAs are presented only in the soma of the Purkinje cells. Double RNAscope showed none of Drp1 mRNAs were co-localized with Mcu mRNAs, as well as almost none of Ucp2 mRNAs were co-localized with Mfn2 mRNAs. All of these results showed the mitochondrial Drp1/Mfn2/Ucp4 convergence on the Purkinje cells. Finally, present research focuses on developing new and more specific molecules tuning the activity of the Purkinje cells activate or inactivate and opening therapeutic windows for Purkinje cells-related diseases. The molecular identification of potential drug targets, mechanism of action, and structural basis of their activity will crucially enable preclinical development.

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“…Our previous study has shown that Drp1 is highly expressed at the spinal cord level [ 33 ]. And many studies have shown different NP contributed to the increased expression of Drp1 [ [34] , [35] , [36] , [37] , [38] , [39] , [40] , [41] , [42] ].…”

Section: Resultsmentioning

confidence: 99%

“…The dynamin family of large GTPases regulates mitochondrial membrane dynamics in all eukaryotes: Drp1 for fission, and mitofusins (Mfn1/2) and optic atrophy-1 (Opa1) for fusion [ [20] , [21] , [22] , [23] ]. Our own study has shown that Drp1 is distributed all over the whole nervous system, especially high at the spinal cord level [ 33 ]. In different NP model, Drp1 expression or its phosphorylated state is reported to either increase or decrease.…”

Section: Discussionmentioning

confidence: 99%

Targeted up-regulation of Drp1 in dorsal horn attenuates neuropathic pain hypersensitivity by increasing mitochondrial fission

Zhang

et al. 2022

Redox Biology

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Mitochondria play an essential role in pathophysiology of both inflammatory and neuropathic pain (NP), but the mechanisms are not yet clear. Dynamin-related protein 1 (Drp1) is broadly expressed in the central nervous system and plays a role in the induction of mitochondrial fission process. Spared nerve injury (SNI), due to the dysfunction of the neurons within the spinal dorsal horn (SDH), is the most common NP model. We explored the neuroprotective role of Drp1 within SDH in SNI. SNI mice showed pain behavior and anxiety-like behavior, which was associated with elevation of Drp1, as well as increased density of mitochondria in SDH. Ultrastructural analysis showed SNI induced damaged mitochondria into smaller perimeter and area, tending to be circular. Characteristics of vacuole in the mitochondria further showed SNI induced the increased number of vacuole, widened vac-perimeter and vac-area. Stable overexpression of Drp1 via AAV under the control of the Drp1 promoter by intraspinal injection (Drp1 OE) attenuated abnormal gait and alleviated pain hypersensitivity of SNI mice. Mitochondrial ultrastructure analysis showed that the increased density of mitochondria induced by SNI was recovered by Drp1 OE which, however, did not change mitochondrial morphology and vacuole parameters within SDH. Contrary to Drp1 OE, down-regulation of Drp1 in the SDH by AAV-Drp1 shRNA (Drp1 RNAi) did not alter painful behavior induced by SNI. Ultrastructural analysis showed the treatment by combination of SNI and Drp1 RNAi (SNI + Drp1 RNAi) amplified the damages of mitochondria with the decreased distribution density, increased perimeter and area, as well as larger circularity tending to be more circular. Vacuole data showed SNI + Drp1 RNAi increased vacuole density, perimeter and area within the SDH mitochondria. Our results illustrate that mitochondria within the SDH are sensitive to NP, and targeted mitochondrial Drp1 overexpression attenuates pain hypersensitivity. Drp1 offers a novel therapeutic target for pain treatment.

show abstract

Drp1 is widely, yet heterogeneously, distributed in the mouse central nervous system

Cited by 11 publications

References 52 publications

Visualizing an convergence of three mitochondrial molecule mRNAs for DRP1/MFN2/UCP4 on soma of cerebellar Purkinje cells by RNAscope

Visualizing an convergence of three mitochondrial molecule mRNAs for DRP1/MFN2/UCP4 on soma of cerebellar Purkinje cells by RNAscope

Visualizing a Convergence of Three Mitochondrial Molecule mRNAs for Drp1/Mfn2/Ucp4 on Soma of Cerebellar Purkinje Cells by RNAscope

Targeted up-regulation of Drp1 in dorsal horn attenuates neuropathic pain hypersensitivity by increasing mitochondrial fission

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