Sep
5
2023
A once-mysterious neural pathway may have a crucial role in making injured areas overly sensitive to touch, a study in mice suggests.
When a person has any kind of injury — a broken shin, for example, or a sunburn — the pain system becomes hypersensitized, firing up in response to normally painless sensations induced by, for instance, walking or a gentle massage. Normally, this tenderness protects the vulnerable tissue as it heals. But occasionally the pain can overstay its usefulness, becoming chronic in conditions such as arthritis.
Now, neuroscientists Robert Edwards and Allan Basbaum from the University of California, San Francisco, and their colleagues have found that a small subset of nerve fibres, the function of which remained a puzzle since their discovery decades ago1, could be routing innocuous touch sensations to the pain pathway when there’s an injury.
“Surprise would be an understatement,” says Basbaum, referring to the findings. “No one knew anything about what these fibres were doing.”
The team’s findings are published by Nature2.
Getting touchy
The researchers found that the fibres, called unmyelinated low-threshold mechanoreceptors (C-LTMRs), are easily stimulated, unlike classic pain fibres, which respond only when the sensation is intense. But C-LTMRs aren’t usually used to detect light touch — this falls to another another major group of sensory neurons — so their role was unclear. The small population of cells have remained enigmatic because they have been difficult to target specifically.
The authors cleared that hurdle when they discovered that these fibres express VGLUT3, a protein necessary for the cells to send signals to other neurons. Because all of the other sensory neurons going to the spinal cord use a different protein — VGLUT1 or VGLUT2 — the authors could engineer mice lacking VGLUT3 to render all the C-LTMRs silent.
“Surprise would be an understatement. No one knew anything about what these fibres were doing.”
Allan Basbaum UCSF
Mice without functional C-LTMRs responded in exactly the same way as normal mice when exposed to light touch and to most painful stimuli, including extreme cold or heat or being poked in the paw with thin wires. But then the authors tested how the mice responded after being injured in three other ways: by a chemical that causes inflammation, which occurs in situations ranging from muscle injuries to a misaligned back; an incision, mimicking pain after surgery; and nerve damage.
In all three types of injury, normal mice became much more sensitive to wires poking their paws, quickly flicking the wires away. But mice with silent C-LTMRs showed much the same responses as before they were injured. All mice, however, became more sensitive to heat, suggesting that the C-LTMRs were hypersensitizing the animals to touch rather than to temperature.
There was one type of pain that, without injury, the engineered mice were less sensitive to than normal mice: intense, persistent pain, such as that caused by a clip pinching the tail. The finding seems contradictory, because C-LTMRs are easily stimulated. One possibility is that a small minority of neurons with VGLUT3 respond to pain, Basbaum says.
Paths to pain
Before this study, researchers had demonstrated two ways for animals to become hypersensitive after injury. First, sensory fibres can become more sensitive to stimulation; this is thought to lead to temperature hypersensitization, as happens when sunburn makes a warm shower feel excruciatingly hot. Second, another set of fibres that, like C-LTMRs, have a low threshold and are important for detecting light touch, are believed to be recruited into the spinal cord’s pain circuit — any sensation they transmit is then perceived as painful.
“This paper says hold on, there’s a whole other population. It’s another circuit, a potential target from a clinical perspective,” says Basbaum. Basbaum thinks that injury also leads to these fibres’ recruitment into the pain circuitry; they may work with the other low-threshold touch fibres or be important for hypersensitivity to different stimuli.
“We knew these fibres existed, but their function was not at all clear until now,” says neuroscientist Clifford Woolf at Harvard Medical School in Boston, Massachusetts. “The data show that recruitment of these fibres is a new way of producing mechanical hypersensitivity. It’s an exciting example of the specific functions of different sets of sensory neurons.
http://www.nature.com/news/2009/091115/full/news.2009.1084.html
Sep
5
2023
The effect of soft tissue release on delayed onset muscle soreness: A pilot study
Dominic Micklewright, Department of Biological Sciences, The University of Essex, Wivenhoe Park, Colchester, Essex CO4 3SQ, UK
Objectives
To examine soft tissue release (STR) as an intervention for delayed onset muscle soreness (DOMS).
Soft tissue release (STR) has been developed (Sanderson, 2002) that involves applying deep pressure to a muscle while simultaneously performing a controlled muscle lengthening by moving the corresponding joint either passively or actively. Unlike many other massage techniques, STR provides a method of manipulating deep tissues throughout the full joint range of motion (Sanderson, 2002). Since the signs and symptoms of exercise induced muscle damage are often more severe towards the limits of joint range of motion, it is conceivable that such signs and symptoms could be targeted more precisely by using STR rather than other types of massage.
Design
A mixed-subjects experimental design was used. Participants performed 4 × 20 eccentric elbow extensions at 80% of 1RM. Participants received either STR (50%) or no treatment (50%). DOMS measurements were taken before the elbow extensions and at 0, 24, and 48 h afterwards.
Setting
The study was conducted at the University of Essex exercise physiology laboratory.
Participants
Twenty male participants, unaccustomed to strength conditioning, completed the study.
Main outcome measures
DOMS was evaluated using relaxed joint angle (RJA), active range of motion (AROM), passive range of motion (PROM), and arm girth measurements. Soreness ratings were measured using a 100 mm visual analogue scale (VAS).
Results
In both conditions there were post-DOMS task increases in VAS ratings (p < 0.0001) and arm girths (p < 0.0001), and decreases in RJA (p < 0.0001), AROM (p < 0.0001), and PROM (p < 0.0001). STR group VAS scores were higher immediately (p < 0.01) and 48 h after treatment (p < 0.005). There were no other between-group differences and none of the measurements returned to baseline levels by 48 h.
Conclusions
STR exacerbates the DOMS sensation yet does not seem to improve the rate of recovery during the first 48 h. What our study adds is that deep aggressive manipulation of damaged muscles, characteristic of STR, does not appear to improve recovery from DOMS. Athletes or rehabilitation practitioners who are looking for a quick fix to DOMS are therefore unlikely to find STR any more useful than more gentle massage techniques. Further research is needed to look more closely at the relationship between manual manipulation of injured tissues and the underlying cellular mechanisms of tissue repair. Without this additional information it is unlikely that the ambiguities surrounding the efficacy of massage and other manual manipulation techniques will be resolved.
Physical Therapy in Sport
Volume 10, Issue 1, February 2009, Pages 19-24
Sep
5
2023
Frankincense may help reduce the symptoms of osteoarthritis, according to a study of 70 patients.
An enriched extract of the “Indian Frankincense” herb Boswellia serrata was used in the randomized, double-blinded, placebo-controlled study. Patients who took the herbal remedy showed significant improvement in as little as seven days. The compound caused no major adverse effects and is safe for human consumption and long-term use, according to the study authors.
The findings were published in the July 29 edition of Arthritis Research & Therapy.
The extract used in the study was enriched with 30 percent AKBA (3-O-acetyl-11-keto-beta-boswellic acid), which is believed to be the most active ingredient in the B. serrata plant.
“AKBA has anti-inflammatory properties, and we have shown that B. serrata enriched with AKBA can be an effective treatment for osteoarthritis of the knee,” study leader Siba Raychaudhuri, a faculty member of the University of California, Davis, said.
“The high incidence of adverse effects associated with currently available medications has created great interest in the search for an effective and safe alternative treatment,” Raychaudhuri said.
B. serrata has been used for thousands of years in traditional Indian medicine. This is the first study to examine the effect of an enriched extract of the plant.
