Pain and Sickle Cell Disease

Overview

Journal Curr Opin Hematol

Specialty Hematology

Date 2019 Mar 21

PMID 30893088

Citations 16

Authors

Anupam Aich

Michael K Jones

Kalpna Gupta

Affiliations

Soon will be listed here.

Abstract

Purpose Of Review: Pain is a major comorbidity of sickle cell disease (SCD). Opioids are the mainstay for pain treatment but remain suboptimal. We discuss mechanism-based treatable targets devoid of opioids to prevent and/or treat SCD pain.

Recent Findings: Understanding the pathogenesis of pain is critical to develop targeted therapies. Nevertheless, acute and chronic pain can have independent and/or overlapping mechanisms. The origin of pain involves neurovascular and neuroimmune interactions from the periphery and/or central nervous system. Immunomodulatory components of acute and/or chronic sickle pain for targeting/preventing pain genesis include mast cell and microglial activation, neurogenic inflammation, and leukocyte-derived elastase. Vascular modulators include hypoxia/reperfusion injury, oxidative stress, hemolysis, and adhesion molecules. However, existent pain requires analgesics devoid of an inadvertent effect on sickle pathobiology. Recent analgesic targets include cannabinoid and nociceptin receptors and serotonergic spinothalamic pathway. Complementary approaches (e.g., acupuncture, hypnosis, perception-based therapies) have shown analgesic potential. Owing to heterogeneity in pain development, it remains challenging to combat SCD pain with any one therapy.

Summary: SCD pain involves neuroimmune and neurovascular interactions. Such interactions have pronociceptive impacts and impart therapy resistance. Elucidating molecular and cellular entities affecting neuronal interactions in sickle microenvironment may prevent SCD pain and/or provide improved analgesic approaches.

Citing Articles

Unmet Need: Mechanistic and Translational Studies of Sickle Cell Disease Pain as a Whole-Person Health Challenge.

Belfer I, Chen W, Weber W, Edwards E, Langevin H J Pain. 2024; 25(10):104603.

PMID: 38878809 PMC: 11402567. DOI: 10.1016/j.jpain.2024.104603.

Hemoglobin scavenger receptor CD163 as a potential biomarker of hemolysis-induced hepatobiliary injury in sickle cell disease.

Kaminski T, Sivanantham A, Mozhenkova A, Smith A, Ungalara R, Dubey R Am J Physiol Cell Physiol. 2024; 327(2):C423-C437.

PMID: 38682236 PMC: 11427010. DOI: 10.1152/ajpcell.00386.2023.

A bone to pick-cellular and molecular mechanisms of bone pain in sickle cell disease.

Gollamudi J, Karkoska K, Gbotosho O, Zou W, Hyacinth H, Teitelbaum S Front Pain Res (Lausanne). 2024; 4:1302014.

PMID: 38239327 PMC: 10794347. DOI: 10.3389/fpain.2023.1302014.

Precision, integrative medicine for pain management in sickle cell disease.

Smith W, Valrie C, Jaja C, Kenney M Front Pain Res (Lausanne). 2023; 4:1279361.

PMID: 38028431 PMC: 10666191. DOI: 10.3389/fpain.2023.1279361.

High Heme and Low Heme Oxygenase-1 Are Associated with Mast Cell Activation/Degranulation in HIV-Induced Chronic Widespread Pain.

Chatterjee T, Arora I, Underwood L, Gryshyna A, Lewis T, Masjoan Juncos J Antioxidants (Basel). 2023; 12(6).

PMID: 37371943 PMC: 10295513. DOI: 10.3390/antiox12061213.