Itch-Associated Peptides: RNA-Seq and Bioinformatic Analysis of Natriuretic Precursor Peptide B and Gastrin Releasing Peptide in Dorsal Root and Trigeminal Ganglia, and the Spinal Cord

Goswami, Samridhi C.; Thierry-Mieg, Danielle; Thierry‐Mieg, Jean; Mishra, Santosh K.; Hoon, Mrinalini; Mannes, Andrew J.; Iadarola, Michael J.

doi:10.1186/1744-8069-10-44

Cited by 52 publications

(54 citation statements)

References 30 publications

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“…It is of interest to note that the number of GRP-positive nerve fibers is higher in the skin of NC/Nga mice, an animal model of atopic dermatitis (Tominaga et al, 2009). On the other hand, Goswami et al (2014) raised a concern that GRP immunoreactivity observed in the dorsal horn may be attributed to cross-reactivity between GRP antiserum and SP or CGRP. To minimize potential cross-reactivity between PNX antiserum and peptides other than phoenixin, a pre-absorption protocol was implemented in which cross-reactivity of PNX antiserum with SP, GRP, CGRP and PNX-14 was individually assessed.…”

Section: Discussionmentioning

confidence: 99%

Phoenixin: A candidate pruritogen in the mouse

Cowan

Lyu²,

Chen

et al. 2015

Neuroscience

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Phoenixin (PNX) is a 14-amino acid amidated peptide (PNX-14) or an N-terminal extended 20-residue amidated peptide (PNX-20) recently identified in neural and non-neural tissue. Mass spectrometry analysis identified a major peak corresponding to PNX-14, with negligible PNX-20, in mouse spinal cord extracts. Using a previously characterized antiserum that recognized both PNX-14 and PNX-20, PNX-immunoreactivity (irPNX) was detected in a population of dorsal root ganglion (DRG) cells and in cell processes densely distributed to the superficial layers of the dorsal horn; irPNX cell processes were also detected in the skin. The retrograde tracer, Fluorogold, injected subcutaneously (s.c.) to the back of the cervical and thoracic spinal cord of mice, labeled a population of DRG, some of which were also irPNX. PNX-14 (2, 4 and 8 mg/kg) injected s.c.to the nape of the neck provoked dose-dependent repetitive scratching bouts directed to the back of the neck with the hindpaws. The number of scratching bouts varied from 16–95 in 30 min, commencing within 5 min post-injection and lasted 10–15 min. Pretreatment of mice at −20 min with nalfurafine (20 µg/kg, s.c.), the kappa opioid receptor agonist, significantly reduced the number of bouts induced by PNX-14 (4 mg/kg) compared with that of saline-pretreated mice. Our results suggest that the peptide, PNX-14, serves as one of the endogenous signal molecules transducing itch sensation in the mouse.

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Section: Discussionmentioning

confidence: 99%

Phoenixin: A candidate pruritogen in the mouse

Cowan

Lyu²,

Chen

et al. 2015

Neuroscience

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“…Detailed information about these donors has been previously described (38, 40). Three female human medullary dorsal horn samples were collected at the level of the pyramidal decussation, and gray matter of the dorsal horn was isolated from fresh tissue by dissection as part of the collection procedure from the National Institute of Mental Health Human Brain Collection Core as described in (40). Rat and human samples were homogenized in QIAzol reagent (Qiagen Inc.) using a FastPrep-24 homogenizer (MP Biomedicals) or using a Polytron homogenizer (IKA) and purified using the RNeasy Mini Kit (Qiagen Inc.) with deoxyribonuclease digestion.…”

Section: Methodsmentioning

confidence: 99%

A systems approach for discovering linoleic acid derivatives that potentially mediate pain and itch

et al. 2017

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Chronic pain and itch are common hypersensitivity syndromes that are affected by endogenous mediators. We applied a systems-based, translational approach to predict, discover, and characterize mediators of pain and itch that are regulated by diet and inflammation. Profiling of tissue-specific precursor abundance and biosynthetic gene expression predicted that inflamed skin would be abundant in four previously unknown 11-hydroxy-epoxy-or 11-keto-epoxy-octadecenoate linoleic acid derivatives and four previously identified 9- or 13-hydroxy-epoxy- or 9- or 13-keto-epoxy-octadecenoate linoleic acid derivatives. All of these mediators were confirmed to be abundant in rat and human skin by mass spectrometry. However, only the two 11-hydroxy-epoxy-octadecenoates sensitized rat dorsal root ganglion neurons to release more calcitonin gene–related peptide (CGRP), which is involved in pain transmission, in response to low pH (which mimics an inflammatory state) or capsaicin (which activates ion channels involved in nociception). The two 11-hydroxy-epoxy-octadecenoates share a 3-hydroxy-Z-pentenyl-E-epoxide moiety, thus suggesting that this substructure could mediate nociceptor sensitization. In rats, intradermal hind paw injection of 11-hydroxy-12,13-trans-epoxy-(9Z)-octadecenoate elicited C-fiber–mediated sensitivity to thermal pain. In a randomized trial testing adjunctive strategies to manage refractory chronic headaches, reducing the dietary intake of linoleic acid was associated with decreases in plasma 11-hydroxy-12,13-trans-epoxy-(9Z)-octadecenoate, which correlated with clinical pain reduction. Human psoriatic skin had 30-fold higher 9-keto-12,13-trans-epoxy-(10E)-octadecenoate compared to control skin, and intradermal injection of this compound induced itch-related scratching behavior in mice. Collectively, these findings define a family of endogenous mediators with potential roles in pain and itch.

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“…RPKM, Reads Per Kilobase of exon model per Million mapped reads, reflects the effect of sequencing depth and unigene length for the read counts at the same time, and is currently the most widely used method to estimate gene expression levels (Agarwal et al, 2010;Ayoub et al, 2011;Goswami et al, 2014;Mortazavi et al, 2008;Sultan et al, 2012;Trapnell et al, 2009;X.O. Zhang et al, 2014).…”

Section: Quantification Of Gene Expression Levelmentioning

confidence: 97%