Your search keyword '"Jiang, Haowu"' showing total 5 results

1. RETRACTED ARTICLE: Targeting KDM1B-dependent miR-215-AR-AGR2-axis promotes sensitivity to enzalutamide-resistant prostate cancer

Author

Tang, Donge, He, Jiaxi, Dai, Yong, Geng, Xinyan, Leng, Qixin, Jiang, Haowu, Sun, Rui, and Xu, Songhui

Abstract

Post-translational modifications of histones by histone demethylases plays an important role in the regulation of gene transcription and are implicated in cancers. Castrate resistant prostate cancer (CRPC) is often driven by constitutively active androgen receptor and commonly becomes resistant to established hormonal therapy strategies such as enzalutamide as a result. However, the role of KDM1B involved in next generation anti-enzalutamide resistance and the mechanisms of KDM1B regulation are poorly defined. Here, we show that KDM1B is upregulated and correlated with prostate cancer progression and poor prognosis. Downregulation of miR-215 is correlated with overexpression of KDM1B in enzalutamide-resistant prostate cancer cells, which promotes AR-dependent AGR2 transcription and regulates the sensitivity to next generation AR-targeted therapy. Inhibition of KDM1B significantly inhibits prostate tumor growth and improves enzalutamide treatments through AGR2 suppression. Our studies demonstrate inhibition of KDM1B can offer a viable therapeutic option to overcome enzalutamide resistance in tumors with deregulated miR-215-KDM1B-AR-AGR2 signaling axis.

Published

2022

2. TRPC3 Antagonizes Pruritus in a Mouse Contact Dermatitis Model

Author

Beattie, Katherine, Jiang, Haowu, Gautam, Mayank, MacVittie, Mary K., Miller, Barbara, Ma, Minghong, Liu, Qin, and Luo, Wenqin

Abstract

Contact dermatitis (CD), including allergic and irritant CD, are common dermatological diseases and are characterized by an erythematous rash and severe itch. In this study, we investigated the function of TRPC3, a canonical transient receptor potential channel highly expressed in type 1 nonpeptidergic (NP1) nociceptive primary afferents and other cell types, in a mouse CD model. Although TrpC3null mice had little deficits in acute somatosensation, they showed significantly increased scratching with CD. In addition, TrpC3null mice displayed no differences in mechanical and thermal hypersensitivity in an inflammatory pain model, suggesting that this channel preferentially functions to antagonize CD-induced itch. Using dorsal root ganglia and panimmune-specific TrpC3conditional knockout mice, we determined that TrpC3in dorsal root ganglia neurons but not in immune cells is required for this phenotype. Furthermore, the number of MRGPRD+NP1 afferents in CD-affected dorsal root ganglia is significantly reduced in TrpC3-mutant mice. Taken together, our results suggest that TrpC3plays a critical role in NP1 afferents to cope with CD-induced excitotoxicity and that the degeneration of NP1 fibers may lead to an increased itch of CD. Our study identified a role of TrpC3and NP1 afferents in CD pathology.

Published

2022

3. Pain and itch coding mechanisms of polymodal sensory neurons

Author

Guo, Changxiong, Jiang, Haowu, Huang, Cheng-Chiu, Li, Fengxian, Olson, William, Yang, Weishan, Fleming, Michael, Yu, Guang, Hoekel, George, Luo, Wenqin, and Liu, Qin

Abstract

Pain and itch coding mechanisms in polymodal sensory neurons remain elusive. MrgprD+neurons represent a major polymodal population and mediate both mechanical pain and nonhistaminergic itch. Here, we show that chemogenetic activation of MrgprD+neurons elicited both pain- and itch-related behavior in a dose-dependent manner, revealing an unanticipated compatibility between pain and itch in polymodal neurons. While VGlut2-dependent glutamate release is required for both pain and itch transmission from MrgprD+neurons, the neuropeptide neuromedin B (NMB) is selectively required for itch signaling. Electrophysiological recordings further demonstrated that glutamate synergizes with NMB to excite NMB-sensitive postsynaptic neurons. Ablation of these spinal neurons selectively abolished itch signals from MrgprD+neurons, without affecting pain signals, suggesting a dedicated itch-processing central circuit. These findings reveal distinct neurotransmitters and neural circuit requirements for pain and itch signaling from MrgprD+polymodal sensory neurons, providing new insights on coding and processing of pain and itch.

Published

2023

4. Retraction Note: Targeting KDM1B-dependent miR-215-AR-AGR2-axis promotes sensitivity to enzalutamide-resistant prostate cancer

Author

Tang, Donge, He, Jiaxi, Dai, Yong, Geng, Xinyan, Leng, Qixin, Jiang, Haowu, Sun, Rui, and Xu, Songhui

Published

2023

5. Anatomical and functional dichotomy of ocular itch and pain

Author

Huang, Cheng-Chiu, Yang, Weishan, Guo, Changxiong, Jiang, Haowu, Li, Fengxian, Xiao, Maolei, Davidson, Steve, Yu, Guang, Duan, Bo, Huang, Tianwen, Huang, Andrew J. W., and Liu, Qin

Abstract

Itch and pain are refractory symptoms of many ocular conditions. Ocular itch is generated mainly in the conjunctiva and is absent from the cornea. In contrast, most ocular pain arises from the cornea. However, the underlying mechanisms remain unknown. Using genetic axonal tracing approaches, we discover distinct sensory innervation patterns between the conjunctiva and cornea. Further genetic and functional analyses in rodent models show that a subset of conjunctival-selective sensory fibers marked by MrgprA3 expression, rather than corneal sensory fibers, mediates ocular itch. Importantly, the actions of both histamine and nonhistamine pruritogens converge onto this unique subset of conjunctiva sensory fibers and enable them to play a key role in mediating itch associated with allergic conjunctivitis. This is distinct from skin itch, in which discrete populations of sensory neurons cooperate to carry itch. Finally, we provide proof of concept that selective silencing of conjunctiva itch-sensing fibers by pruritogen-mediated entry of sodium channel blocker QX-314 is a feasible therapeutic strategy to treat ocular itch in mice. Itch-sensing fibers also innervate the human conjunctiva and allow pharmacological silencing using QX-314. Our results cast new light on the neural mechanisms of ocular itch and open a new avenue for developing therapeutic strategies.

Published

2018