Temporomandibular Joint Disorder Clinical Trial
Official title:
Biobehavioral Pain Management in TMD
TMD is a poorly understood chronic pain disorder that affects up to 15% of the adult
population, notably impacting women, is linked to greater healthcare utilization, and
associated with multiple pain-related co-morbidities. Pain-related catastrophizing (CAT) and
sleep continuity disturbance (SCD) are well established modifiable risk factors for TMD and
other idiopathic pain conditions. Neither the causal status nor the neurobiological
mechanisms by which these factors exert their effects on clinical pain have been established.
We propose that CAT and SCD influence clinical pain through shared alterations in pain
modulation and key neurobiological pathways, including amplified inflammatory activity,
autonomic activity, and adrenocortical functioning. Beyond these shared mechanisms, however,
we propose to determine whether pre-sleep CAT increases cortical arousal during sleep. The
cognitive dimensions of pre-sleep arousal, particularly rumination and negative sleep-related
thoughts, are central to the phenomenology of insomnia. Extending this notion, we propose
that CAT in those experiencing ongoing clinical pain fosters sleep disturbance owing to
increased pre- and peri-sleep cognitive arousal. Moreover, we propose that pre-sleep CAT is
related to subtle variations in objective indices of fragmented sleep (e.g., cortical
arousal). We will examine key hypotheses derived from this framework using a brief,
prospective randomized experiment, which will permit careful analysis of the temporal
patterning of how changes in either CAT or SCD influence each other and contribute to
alterations in pain modulatory systems, key nociceptive mechanisms, and clinical pain.
Women experiencing at least moderate chronic TMD pain (N=225) who demonstrate at least mild
trait catastrophizing and meet at least subclinical insomnia criteria (SCD) will be randomly
assigned to: 1) cognitive therapy for catastrophizing (CT-CAT); 2) behavior therapy for sleep
disturbance (BT-SCD); or 3) TMD education (Control). Assessments of clinical pain, sleep
disturbance, catastrophizing, pain sensitivity and modulatory systems, and indices of
inflammatory activity, adrenocortical function and autonomic balance will be completed at
baseline, 4 weeks (mid-manipulation) and 8 weeks (post-manipulation). Clinical pain, sleep,
catastrophizing and covariates will additionally be measured at 16 weeks (follow-up).
Temporomandibular Joint Disorder (TMJD) is a poorly understood chronic pain disorder
characterized by pain and dysfunction in the jaw joint and the muscles that control jaw
movement. TMJD affects up to 15% of the adult population, differentially impacts women, is
linked to greater healthcare utilization, and is associated with multiple pain-related
co-morbidities. Pain-related catastrophizing (i.e., the tendency to exaggerate the threat
value of pain and negatively evaluate one's ability to deal with pain; CAT) and sleep
continuity disturbance (i.e., disturbance in the speed with which sleep is initiated and the
degree to which it is consolidated; SCD) are two well established modifiable risk factors for
TMJD and other idiopathic pain conditions. SCD is defined in this protocol as at least
moderate trouble initiating or maintaining sleep, which significantly impacts daytime
function. SCD is common in chronic pain, including TJMD, and poor sleep predicts both the
development and exacerbation of pain. CAT, a negative cognitive-emotional predilection and
response to pain, prospectively predicts the onset and exacerbation of pain, as well as
numerous pain-related outcomes. Surprisingly, neither the causal status nor the
neurobiological mechanisms by which these factors exert their effects on clinical pain have
been established. Preliminary data from our group and others suggest that CAT and SCD are
independently associated with alterations in laboratory indices of pain modulation,
exaggerated pain-evoked pro-inflammatory cytokine responses and amplified clinical pain.
While the effects of CAT and SCD are independent of depression and psychological distress, no
longitudinal or experimental studies have evaluated the potential interplay between CAT and
SCD and how this interplay contributes to pain outcomes. There is a strong theoretical reason
to hypothesize interplay between these seemingly disparate constructs among patients with
chronic pain. We have developed a novel, integrated theoretical framework positing that CAT
and SCD influence clinical pain through shared alterations in pain modulation and key
neurobiological pathways, including amplified inflammatory activity, sympathetic activity,
and adrenocortical functioning. Beyond these shared mechanisms, however, we propose to
determine whether presleep CAT increases autonomic and cortical arousal during sleep measured
by polysomnography (PSG)-derived indices of Heart Rate Variability (HRV) and average relative
power in the alpha and beta bands on quantitative electroencephalography (QEEG). The
cognitive dimensions of pre-sleep arousal, particularly rumination and negative sleep-related
thoughts, are central to the phenomenology of insomnia. Extending this notion, we propose
that CAT in those experiencing ongoing clinical pain fosters sleep disturbance owing to
increased pre- and peri-sleep cognitive arousal. Moreover, we propose that pre-sleep CAT is
related to subtle variations in objective indices of fragmented sleep (e.g., cortical
arousal). We will examine key hypotheses derived from this framework using a brief,
prospective randomized experiment, which will permit careful analysis of the temporal
patterning of how changes in either CAT or SCD influence each other and contribute to
alterations in pain modulatory systems, key nociceptive mechanisms, and clinical pain.
In this 5 year study, 300 women with chronic TMJD and reporting at least mild trait
catastrophizing and at least mild sleep continuity disturbance will complete a randomized,
parallel group experiment comparing cognitive therapy for catastrophizing (CT-CAT) and
behavior therapy for sleep disturbance (BT-SCD) to TMJD disease education (TMJD-ED). Subjects
will be randomized in a ratio of 1:1:1 to one of the three interventions. Each subject will
participate in the study for up to 30 weeks. The study includes three phases: 1) screening
and baseline (up to 10 weeks), 2) intervention (approximately 7 weeks), and 3) follow-up
(ends approximately 12 weeks after the final intervention visit). Assessments of outcome
measures (inflammatory activity, pain modulation, clinical pain, pre-sleep cognitive arousal,
cortical and autonomic arousal) will be made during the interventions and after completion of
the interventions, and will be compared with baseline assessments. It is anticipated that
enrollment will be completed over four years.
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