Lack of association between angiotensin-converting enzyme inhibitors and angiotensin receptor blockers and pain improvement in patients with oral cancer

Du, Kim; Shepherd, Andrew J.; Irvin, Veronica L.; Roldan, Carlos J.; Amit, Moran; Feng, Lei; Desai, Shubh; Cata, Juan P.

doi:10.3332/ecancer.2020.1121

Cited by 8 publications

(5 citation statements)

References 29 publications

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“…These results indicate a possible mechanism for the analgesic actions of different AT1R antagonists (see section 3.3) and should be further investigated in relation to NP and other different pain diseases. AT1R antagonists are associated with reduced perineural invasion in head and neck cancer, 35 although it is not yet clear if this is due to an AT1R-mediated effect on chemokine expression. Collectively, these findings are likely to be relevant for NP because leukocyte infiltration and the consequent proinflammatory actions are known to be significant contributors to development and maintenance of NP.…”

Section: Effect Of the Renin–angiotensin System On Immune System Function And Implications For Neuropathic Painmentioning

confidence: 99%

Angiotensin receptors and neuropathic pain

Balogh

Aguilar

Nguyen

et al. 2021

PR9

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Growing evidence implicates the renin–angiotensin system (RAS) in multiple facets of neuropathic pain (NP). This narrative review focuses primarily on the major bioactive RAS peptide, Angiotensin II (Ang II), and its receptors, namely type 1 (AT1R) and type 2 (AT2R). Both receptors are involved in the development of NP and represent potential therapeutic targets. We first discuss the potential role of Ang II receptors in modulation of NP in the central nervous system. Ang II receptor expression is widespread in circuits associated with the perception and modulation of pain, but more studies are required to fully characterize receptor distribution, downstream signaling, and therapeutic potential of targeting the central nervous system RAS in NP. We then describe the peripheral neuronal and nonneuronal distribution of the RAS, and its contribution to NP. Other RAS modulators (such as Ang (1-7)) are briefly reviewed as well. AT1R antagonists are analgesic across different pain models, including NP. Several studies show neuronal protection and outgrowth downstream of AT2R activation, which may lead to the use of AT2R agonists in NP. However, blockade of AT2R results in analgesia. Furthermore, expression of the RAS in the immune system and a growing appreciation of neuroimmune crosstalk in NP add another layer of complexity and therapeutic potential of targeting this pathway. A growing number of human studies also hint at the analgesic potential of targeting Ang II signaling. Altogether, Ang II receptor signaling represents a promising, far-reaching, and novel strategy to treat NP.

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Section: Effect Of the Renin–angiotensin System On Immune System Function And Implications For Neuropathic Painmentioning

confidence: 99%

Angiotensin receptors and neuropathic pain

Balogh

Aguilar

Nguyen

et al. 2021

PR9

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“…In vitro, pancreatic adenocarcinoma cells were shown to induce neurotropism in cultured mouse dorsal root ganglion neurons, and enhanced neurite outgrowth was also associated with greater cancer cell colony growth [ 53 ]. PNI is associated with higher pain intensity [ 54 ], and pain intensity is also a predictor of poor prognosis in head and neck cancers [ 3 ] and non-small cell lung cancers [ 4 ].…”

Section: Mor Biology In Cancermentioning

confidence: 99%

Opioids and Cancer: Current Understanding and Clinical Considerations

Sah,

Shoffel-Havakuk,

Tsur

et al. 2024

Current Oncology

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Pain is one of the most common symptoms in patients with cancer. Pain not only negatively affects the quality of life of patients with cancer, but it has also been associated with reduced survival. Pain management is therefore a critical component of cancer care. Prescription opioids remain the first-line approach for the management of moderate-to-severe pain associated with cancer. However, there has been increasing interest in understanding whether these analgesics could impact cancer progression. Furthermore, epidemiological data link a possible association between prescription opioid usage and cancer development. Until more robust evidence is available, patients with cancer with moderate-to-severe pain may receive opioids to decrease suffering. However, future studies should be conducted to evaluate the role of opioids and opioid receptors in specific cancers.

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“…[75] One of the single most important factors of moderate-tosevere pain in patients with cancer is perineural tumor invasion. [76] This can be defined as cancer cells surrounding more than one-third of the nerve periphery or invading any layer of the neurolemma. [77] Perineural invasion is a complex and dynamic process that requires close and orchestrated interactions between axons, nerve endings, and cancer cells, and it occurs early during tumorigenesis.…”

Section: The Role Of the Tumoral μ-Opioid Receptor In The Cancer-nerv...mentioning

confidence: 99%