Inflammation

Cases studies Activation of pain transmission nerves Muscle contraction Inflammation Nerve root compression

Inflammation essentially consists of a great dilatation of blood vessels next to the opening of the pores, allowing a permeable pathway for fluids, substances and cells from the bloodstream to the tissues; these tissues increase their volume and temperature.

Pain nerve activation induces the release of certain neurotransmitters that dilate vessels and open the pores, causing tissue inflammation along the releasing sites. This is called "neurogenic inflammation". Some of the implicated neurotransmitters are CGRP (calcitonin-gene-related-peptide), NKA (neurokynine A) and Substance P (SP).

Some blood cells are also activated in specific circumstances, especially when they detect the presence of microbes, releasing substances that attract other systemic defense cells, which create vessel and pore dilatation, opening a pathway for these cells to reach tissues. This is known as "humoral inflammation"; some of the released substances are prostaglandins and leukotrienes.

It has been shown that neurogenous and humoral inflammation potentiate each other and that both processes are implicated in back pain. This explains the efficacy of treatment with anti-inflammatory agents, since they hinder prostaglandin production and interfere in the interaction between humoral and neurogenic inflammation.

In back pain, inflammation is essentially a consequence of a release of neurotransmitters, together with pain nerve activation and, secondarily, of the start of a humoral inflammation process. Nevertheless, after the onset of inflammation, this in itself becomes an added aggravating factor:

On the one hand, released substances at the onset of humoral inflammation are able to activate pain nerves, thus increasing pain. At the same time, pain releases the neurotransmitters involved in neurogenic inflammation, which increases inflammation, creating a vicious circle.

On the other hand, at increased tissue volume the risk for nerve compression also increases which in turn worsens the causal lesion. For example, in a disc herniation, inflammation may increase the herniated pulpous material, or decrease the fissure opening of the fibrous fold from where it protruded.