B-type natriuretic peptide is neither itch-specific nor functions upstream of the GRP-GRPR signaling pathway

Xian Yu Liu; Li Wan; Fu Quan Huo; Devin M. Barry; Hui Li; Zhong Qiu Zhao; Zhou Feng Chen

doi:10.1186/1744-8069-10-4

B-type natriuretic peptide is neither itch-specific nor functions upstream of the GRP-GRPR signaling pathway

Xian Yu Liu
, Li Wan
, Fu Quan Huo
, Devin M. Barry
, Hui Li
, Zhong Qiu Zhao
, Zhou Feng Chen

Washington University St. Louis

科研成果: 期刊稿件 › 文章 › 同行评审

64 引用（Scopus）

摘要

Background: A recent study by Mishra and Hoon identified B-type natriuretic peptide (BNP) as an important peptide for itch transmission and proposed that BNP activates spinal natriuretic peptide receptor-A (NPRA) expressing neurons, which release gastrin releasing peptide (GRP) to activate GRP receptor (GRPR) expressing neurons to relay itch information from the periphery to the brain (Science 340:968-971, 2013). A central premise for the validity of this novel pathway is the absence of GRP in the dorsal root ganglion (DRG) neurons. To this end, they showed that Grp mRNA in DRG neurons is either absent or barely detectable and claimed that BNP but not GRP is a major neurotransmitter for itch in pruriceptors. They showed that NPRA immunostaining is perfectly co-localized with Grp-eGFP in the spinal cord, and a few acute pain behaviors in Nppb^-/-mice were tested. They claimed that BNP is an itch-selective peptide that acts as the first station of a dedicated neuronal pathway comprising a GRP-GRPR cascade for itch. However, our studies, along with the others, do not support their claims.Findings: We were unable to reproduce the immunostaining of BNP and NPRA as shown by Mishra and Hoon. By contrast, we were able to detect Grp mRNA in DRGs using in situ hybridization and real time RT-PCR. We show that the expression pattern of Grp mRNA is comparable to that of GRP protein in DRGs. Pharmacological and genetic blockade of GRP-GRPR signaling does not significantly affect intrathecal BNP-induced scratching behavior. We show that BNP inhibits inflammatory pain and morphine analgesia.Conclusions: Accumulating evidence demonstrates that GRP is a key neurotransmitter in pruriceptors for mediating histamine-independent itch. BNP-NPRA signaling is involved in both itch and pain and does not function upstream of the GRP-GRPR dedicated neuronal pathway. The site of BNP action in itch and pain and its relationship with GRP remain to be clarified.

源语言	英语
文章编号	4
期刊	Molecular Pain
卷	10
期	1
DOI	https://doi.org/10.1186/1744-8069-10-4
出版状态	已出版 - 18 1月 2014
已对外发布	是

访问文件

10.1186/1744-8069-10-4

其它文件与链接

链接到 Scopus 的出版物

引用此

@article{aa828706d4cb41c38eaa2e6fcb1dca00,

title = "B-type natriuretic peptide is neither itch-specific nor functions upstream of the GRP-GRPR signaling pathway",

abstract = "Background: A recent study by Mishra and Hoon identified B-type natriuretic peptide (BNP) as an important peptide for itch transmission and proposed that BNP activates spinal natriuretic peptide receptor-A (NPRA) expressing neurons, which release gastrin releasing peptide (GRP) to activate GRP receptor (GRPR) expressing neurons to relay itch information from the periphery to the brain (Science 340:968-971, 2013). A central premise for the validity of this novel pathway is the absence of GRP in the dorsal root ganglion (DRG) neurons. To this end, they showed that Grp mRNA in DRG neurons is either absent or barely detectable and claimed that BNP but not GRP is a major neurotransmitter for itch in pruriceptors. They showed that NPRA immunostaining is perfectly co-localized with Grp-eGFP in the spinal cord, and a few acute pain behaviors in Nppb-/-mice were tested. They claimed that BNP is an itch-selective peptide that acts as the first station of a dedicated neuronal pathway comprising a GRP-GRPR cascade for itch. However, our studies, along with the others, do not support their claims.Findings: We were unable to reproduce the immunostaining of BNP and NPRA as shown by Mishra and Hoon. By contrast, we were able to detect Grp mRNA in DRGs using in situ hybridization and real time RT-PCR. We show that the expression pattern of Grp mRNA is comparable to that of GRP protein in DRGs. Pharmacological and genetic blockade of GRP-GRPR signaling does not significantly affect intrathecal BNP-induced scratching behavior. We show that BNP inhibits inflammatory pain and morphine analgesia.Conclusions: Accumulating evidence demonstrates that GRP is a key neurotransmitter in pruriceptors for mediating histamine-independent itch. BNP-NPRA signaling is involved in both itch and pain and does not function upstream of the GRP-GRPR dedicated neuronal pathway. The site of BNP action in itch and pain and its relationship with GRP remain to be clarified.",

keywords = "BNP, DRG, GRP, GRPR, Itch, NPRA, Pain, Spinal cord",

author = "Liu, \{Xian Yu\} and Li Wan and Huo, \{Fu Quan\} and Barry, \{Devin M.\} and Hui Li and Zhao, \{Zhong Qiu\} and Chen, \{Zhou Feng\}",

year = "2014",

month = jan,

day = "18",

doi = "10.1186/1744-8069-10-4",

language = "英语",

volume = "10",

journal = "Molecular Pain",

issn = "1744-8069",

publisher = "SAGE Publications Inc.",

number = "1",

}

TY - JOUR

T1 - B-type natriuretic peptide is neither itch-specific nor functions upstream of the GRP-GRPR signaling pathway

AU - Liu, Xian Yu

AU - Wan, Li

AU - Huo, Fu Quan

AU - Barry, Devin M.

AU - Li, Hui

AU - Zhao, Zhong Qiu

AU - Chen, Zhou Feng

PY - 2014/1/18

Y1 - 2014/1/18

N2 - Background: A recent study by Mishra and Hoon identified B-type natriuretic peptide (BNP) as an important peptide for itch transmission and proposed that BNP activates spinal natriuretic peptide receptor-A (NPRA) expressing neurons, which release gastrin releasing peptide (GRP) to activate GRP receptor (GRPR) expressing neurons to relay itch information from the periphery to the brain (Science 340:968-971, 2013). A central premise for the validity of this novel pathway is the absence of GRP in the dorsal root ganglion (DRG) neurons. To this end, they showed that Grp mRNA in DRG neurons is either absent or barely detectable and claimed that BNP but not GRP is a major neurotransmitter for itch in pruriceptors. They showed that NPRA immunostaining is perfectly co-localized with Grp-eGFP in the spinal cord, and a few acute pain behaviors in Nppb-/-mice were tested. They claimed that BNP is an itch-selective peptide that acts as the first station of a dedicated neuronal pathway comprising a GRP-GRPR cascade for itch. However, our studies, along with the others, do not support their claims.Findings: We were unable to reproduce the immunostaining of BNP and NPRA as shown by Mishra and Hoon. By contrast, we were able to detect Grp mRNA in DRGs using in situ hybridization and real time RT-PCR. We show that the expression pattern of Grp mRNA is comparable to that of GRP protein in DRGs. Pharmacological and genetic blockade of GRP-GRPR signaling does not significantly affect intrathecal BNP-induced scratching behavior. We show that BNP inhibits inflammatory pain and morphine analgesia.Conclusions: Accumulating evidence demonstrates that GRP is a key neurotransmitter in pruriceptors for mediating histamine-independent itch. BNP-NPRA signaling is involved in both itch and pain and does not function upstream of the GRP-GRPR dedicated neuronal pathway. The site of BNP action in itch and pain and its relationship with GRP remain to be clarified.

AB - Background: A recent study by Mishra and Hoon identified B-type natriuretic peptide (BNP) as an important peptide for itch transmission and proposed that BNP activates spinal natriuretic peptide receptor-A (NPRA) expressing neurons, which release gastrin releasing peptide (GRP) to activate GRP receptor (GRPR) expressing neurons to relay itch information from the periphery to the brain (Science 340:968-971, 2013). A central premise for the validity of this novel pathway is the absence of GRP in the dorsal root ganglion (DRG) neurons. To this end, they showed that Grp mRNA in DRG neurons is either absent or barely detectable and claimed that BNP but not GRP is a major neurotransmitter for itch in pruriceptors. They showed that NPRA immunostaining is perfectly co-localized with Grp-eGFP in the spinal cord, and a few acute pain behaviors in Nppb-/-mice were tested. They claimed that BNP is an itch-selective peptide that acts as the first station of a dedicated neuronal pathway comprising a GRP-GRPR cascade for itch. However, our studies, along with the others, do not support their claims.Findings: We were unable to reproduce the immunostaining of BNP and NPRA as shown by Mishra and Hoon. By contrast, we were able to detect Grp mRNA in DRGs using in situ hybridization and real time RT-PCR. We show that the expression pattern of Grp mRNA is comparable to that of GRP protein in DRGs. Pharmacological and genetic blockade of GRP-GRPR signaling does not significantly affect intrathecal BNP-induced scratching behavior. We show that BNP inhibits inflammatory pain and morphine analgesia.Conclusions: Accumulating evidence demonstrates that GRP is a key neurotransmitter in pruriceptors for mediating histamine-independent itch. BNP-NPRA signaling is involved in both itch and pain and does not function upstream of the GRP-GRPR dedicated neuronal pathway. The site of BNP action in itch and pain and its relationship with GRP remain to be clarified.

KW - BNP

KW - DRG

KW - GRP

KW - GRPR

KW - Itch

KW - NPRA

KW - Pain

KW - Spinal cord

UR - https://www.scopus.com/pages/publications/84892462094

U2 - 10.1186/1744-8069-10-4

DO - 10.1186/1744-8069-10-4

M3 - 文章

C2 - 24438367

AN - SCOPUS:84892462094

SN - 1744-8069

VL - 10

JO - Molecular Pain

JF - Molecular Pain

IS - 1

M1 - 4

ER -

B-type natriuretic peptide is neither itch-specific nor functions upstream of the GRP-GRPR signaling pathway

摘要

访问文件

其它文件与链接

学术指纹

引用此