Case Study
A 38-year-old woman with a history of chronic back pain, for which she was not taking any medications except for occasional ibuprofen, and one previous cesarean delivery was scheduled for an anesthetic consultation at 35 weeks’ gestation because she was extremely concerned and somewhat traumatized with her previous delivery experience 2 years ago.
She reported that while her epidural placed for labor analgesia had worked fine, when the obstetrician decided to proceed with a cesarean delivery for failure to progress, the epidural didn’t work that well, and while the anesthesiologist kept telling her that “feeling some pressure is normal during a cesarean delivery,” she felt tremendous pain throughout the surgery and was sure the epidural wasn’t working. She was afraid the anesthesiologist would decide to put to her to sleep and remembered vaguely receiving something intravenously. She also remembered having severe pain, mostly at the level of the incision, for several days after delivery and felt that the medication – IV patient-controlled analgesia (PCA) with morphine – did not help and just made her very nauseous. She reported having persistent pain around the incision for many weeks, with residual numbness and unpleasant “pins and needles” consistent with paresthesia and was extremely worried that she might again experience severe pain during this cesarean delivery and chronic pain after.
On reviewing the medical records from the previous cesarean delivery, it appeared that the epidural catheter had been topped up with 2% lidocaine with epinephrine 1:200,000 in 5-ml incremental boluses, up to a total of 20 ml, along with fentanyl 100 µg, and the reported sensory level to pinprick was T4 bilaterally. IV midazolam 2 mg was given after the baby was born, along with epidural preservative-free morphine 3 mg. Multimodal analgesia with a nonsteroidal anti-inflammatory drug (IV ketorolac followed by oral ibuprofen) and oral acetaminophen was given in the recovery room, and because the patient reported severe pain, IV PCA morphine had also been started.
Key Points
Women may present for obstetric surgery with a history of chronic pain related to a previous delivery with features of persistent neuropathic pain causing significant anxiety and fear of pain.
It is important to reassure such women that all anesthetic and analgesic modalities will be tailored to their needs and to explain the different options for anesthesia and postcesarean analgesia.
Strategies should include a dense neuraxial anesthetic block, with consideration of adjuvants to ensure anxiolysis and antihyperalgesia, such as intrathecal clonidine.
IV ketamine and oral gabapentin may be considered for a prolonged period of time after delivery in an attempt to prevent hypersensitization and worsening of any preexisting neuropathic symptoms.
Discussion
Characteristics of Pain during and after Cesarean Delivery
Most women reporting pain during cesarean delivery complain of “intense pulling and tugging” along with nausea and vomiting, which can be exacerbated by uterine exteriorization1 (which is a common practice in the United States to facilitate uterine exposure and closure) or if bilateral tubal ligation2 is performed during the cesarean delivery; these unpleasant sensations reflect the intense visceral stimuli that accompany manipulation of the peritoneum. Ways to alleviate these sensations are to ensure an adequate dense surgical block up to T4, to be confirmed with pinprick testing, which can be easier to achieve with a spinal anesthetic than with an epidural anesthetic. Short-acting opioids are essential and can be given with the spinal local anesthetic or via an indwelling epidural catheter.3–5 As an additional adjuvant, spinal or epidural clonidine may be used.5 Clonidine has been shown to be extremely effective in reducing intraoperative pain.
Acute pain
during cesarean delivery is an important event to identify and acknowledge because it has been consistently associated with an increased risk of developing persistent postoperative pain (pain that goes beyond the expected time of healing, typically up to 8–12 weeks after surgery, in this case after cesarean delivery).6–11
Chronic postcesarean pain
, or pain that has developed in relation to the cesarean delivery and persists beyond 3 months after delivery, has been established to be quite rare,12 particularly in comparison with other types of surgery, including hysterectomy.13 The proposed mechanism for protection from chronic postcesarean pain is a putative effect of endogenous central oxytocin,14 which was recently investigated in animal models of pain.15, 16 While chronic pain per se is uncommon after cesarean delivery, postoperative symptoms and specifically neuropathic characteristics of pain have been found to be common after cesarean deliveries.11, 17
Neuropathic pain
refers to pain after neural injury (peripheral or central), and a key feature is the combination of sensory loss with paradoxical hypersensitivity, including hypoesthesia (a reduced or partial sensation to touch), dysesthesia (a painful sensation after superficial touch), allodynia (a painful response to a normally innocuous stimuli, often to cold), hyperalgesia (an increased response to noxious stimuli), hyperpathia (an increased and persistent response to noxious stimuli) and burning pain. Not all patients with nerve damage will experience neuropathic pain; the type of nerve injury may explain the increase in both acute and chronic pain, but the extent of pain is mediated by other factors, including genetic, psychological, and physiologic factors that heighten pain sensitivity and impair pain modulation.
Predicting Women at Risk for Pain after Cesarean Delivery
There have been several studies trying to identify which women will be more likely to suffer acute and persistent pain after cesarean delivery. Some have used experimental pain modalities such as quantitative sensory tests (QSTs) to predict women’s risk for intense postcesarean pain.18–24 Problems with such experimental tests is that depending on the pain modality used, these tests may not necessarily accurately predict postpartum pain because of its complex nature (including uterine cramping and postoperative pain). In addition, most of these tests are not easy to perform in a clinical setting and will not be directly useful and applicable to guide clinicians caring for women during cesarean delivery. Questions to assess women’s pain catastrophization,18 level of anxiety, and anticipated pain25 have been shown to predict acute postcesarean pain. Finally, testing women undergoing a repeat cesarean delivery to assess whether some degree of scar hyperalgesia, which reflects hypersensitization, is present prior to surgery has been shown to predict acute postcesarean pain and analgesic consumption in the first 48 hours following the repeated procedure.11 This confirms the concept that central sensitization preceding surgery may impair pain modulation and result in the second surgical procedure, here a repeat cesarean delivery, to cause more severe pain and potentially hyperalgesia and chronic pain. Identifying women with predisposing factors such as preexisting chronic pain, neuropathic symptoms, or other contributors such as psychological or genetic factors will ensure that antihyperalgesic/neuropathic adjuvants be targeted to the subset of women who actually need these additional medications (Figure 40.1).
Anesthetic Options for a Repeat Cesarean Delivery to Reduce Acute Pain and Minimize the Risk for Persistent Postoperative Pain in Women at Risk
1. A single shot spinal (SSS) with
A standard spinal solution with or without clonidine
2. A combined spinal-epidural (CSE) with
A standard spinal solution
Option to top up the epidural catheter intraoperatively if necessary
Option to keep the epidural catheter for postcesarean analgesia
3. Intravenous ketamine intraoperatively
4. Transversus abdominis plane (TAP) block or Quadratus Lumborum block (QLB) for breakthrough pain
5. Prolonged oral gabapentin (see Table 40.1 for drug doses)
Table 40.1 Anesthetic Options for a Repeat Cesarean Delivery to Reduce Acute Pain and Minimize the Risk for Persistent Postoperative Pain in Women at Risk
| Option | Additional adjuvant | |||
|---|---|---|---|---|
| Single-shot spinal (standard spinal dose) | ||||
| Spinal | Hyperbaric Bupivacaine | Fentanyl | Morphine | Clonidine |
| 12 mg | 10–15 µg | 100–300 µg | 60–100 µg | |
| Combined spinal-epidural (CSE) (standard spinal dose followed by epidural dosing) | ||
|---|---|---|
| Epidural | Intraoperatively | |
| Lidocaine 2% + epinephrine 1:200,000 5-20 ml as needed | Clonidine 60–150 µg | |
| Postoperatively | ||
| Solution: Bupivacaine 0.0625% + fentanyl 2 µg/ml for 24–48 hours | ||
| Regimen:1: Continuous epidural infusion (CEI) (8–12 ml) with PCEA (bolus 5-8 ml) | ||
| Regimen 2: Programmed intermittent epidural bolus (PIEB) with PCEA | ||
| May be followed by a dose of epidural morphine 3 mg before epidural catheter is removed or epidural morphine 3 mg (every 18–24 hours) for 24–72 hours | ||
| Transversus abdominis plane (TAP) block / Quadratus Lumborum Block (QLB) | |
|---|---|
| Single-shot TAP | Postoperatively (or on day 1–2 postpartum) |
| Ropivacaine 0.2% or bupivacaine / levobupivacaine 0.25%, 15–20 ml per side | |
| TAP catheters | Postoperatively (or on day 1–2 postpartum) |
| Repeat bolus (see Single-shot TAP) every 8 hours through catheters | |
| QLB | Postoperatively levobupivacaine 0.25% 20 ml per side. |
| Systemic medication | |
|---|---|
| Intravenous | Ketamine 0.15–0.5 mg/kg |
| Oral | Gabapentin 300–600 mg two to three times a day |
| Start at least 2 hours (ideally 48 hours) before cesarean delivery | |
| Duration may be up to 2–3 weeks for maximal effect in preventing neuropathic pain | |
Neuraxial Clonidine
Clonidine is a potent α2-adrenergic receptor agonist with antinociceptive effects acting via descending pathways to the dorsal horn of the spinal cord. It is effective for both somatic and visceral pain.26 Intrathecal clonidine added to local anesthetics for surgery prolongs the surgical block time (sensory regression to L2 and duration of motor block) and the time to first analgesic request.27 Multiple studies have evaluated the effect of intrathecal clonidine on intraoperative analgesia, onset and duration of surgical block, time to first analgesic request, morphine-sparing effect, shivering, and side-effect profile in women receiving varying doses of intrathecal clonidine for elective cesarean delivery.5, 28–35
Taken together, all these studies suggest that adding an “intermediate” dose of clonidine (60–100 µg) prolongs the surgical block by up to 60 minutes, delays the time to first analgesic request for breakthrough pain, and has a beneficial effect on intraoperative shivering.36 None of the studies reported severe hypotension with any of the studied doses, including relatively high doses (150 µg).33, 35 The proposed explanation is that hypotension occurs in almost 100 percent of women immediately after injection of the spinal solution; therefore, adding clonidine will not increase the incidence of hypotension and will be easily managed with the current practice of using a vasopressor infusion (typically phenylephrine) during cesarean delivery. However, because the effect of neuraxial clonidine may outlast the surgical time, maternal blood pressure may remain low in the post-anesthesia care unit (PACU), and maintaining a phenylephrine infusion for a few hours in the PACU may be required in some cases. While the sedative effect of clonidine has been evaluated, the anxiolytic effect of spinal clonidine has not been assessed. It is unclear whether spinal clonidine reduces the likelihood of suffering chronic postcesarean pain, most likely because this event is so uncommon, and much larger studies would be needed to explore this effect or studies that prescreen women to identify those most likely to benefit from the addition of an antihyperalgesic drug. Based on our vast clinical experience with spinal clonidine for cesarean deliveries, clonidine is best suited for women who either already suffer chronic pain, are opioid tolerant, have had a suboptimal experience with a previous cesarean delivery (anesthetic block not sufficiently dense, not lasting long enough, severe postcesarean pain) and/or are extremely anxious.
Intravenous Ketamine
Ketamine, an N-methyl-d-aspartate (NMDA) receptor antagonist, has been suggested as an intraoperative adjuvant to reduce acute postoperative pain, reduce opioid-related side effects, and potentially prevent chronic postoperative pain. Systematic reviews have demonstrated a morphine-sparing effect postoperatively37 but insufficient evidence to support its routine use to prevent chronic pain.38 In a recent systematic review and meta-analysis of the effects of ketamine during cesarean delivery under spinal or general anesthesia,39 ketamine significantly delayed time to first analgesic request and reduced pain scores 2 hours after cesarean delivery under spinal anesthesia.
To our knowledge, no academic center in the United States uses IV ketamine (as a bolus or per infusion) to prevent intraoperative pain at the beginning of the procedure. Current recommendations are not for its routine use, although doses of titrated IV ketamine may be offered to women reporting significant intraoperative pain.
Oral Gabapentin
Preoperative administration of gabapentinoids (gabapentin or pregabalin) to prevent severe acute and chronic postoperative pain has been evaluated.40 In the context of cesarean delivery, only three studies have evaluated the effect of a single preoperative dose of oral gabapentin, with mixed results.41–43 Doses were either 300 mg41, 42 or 600 mg42, 43 taken 2 hours before cesarean delivery. It is possible that both the timing and duration were insufficient for both a morphine-sparing effect and the prevention of neuropathic pain. Starting gabapentinoids 48 hours prior to surgery and for a duration of at least 2–3 weeks to elicit a long-lasting effect has been proposed.40 Women at low risk for severe acute postcesarean pain are unlikely to benefit from the administration of a single oral dose of gabapentin preoperatively, but for selected women at risk for neuropathic pain, prolonged gabapentin may be beneficial.
Regional Truncal Blocks
The transversus abdominis plane (TAP) block is a recently investigated regional technique that is effective and relatively simple to manage. The duration of a single-shot TAP block does not seem to exceed 15–18 hours. Multiple studies have evaluated the efficacy of TAP blocks regarding their opioid-sparing ability, and when compared with spinal morphine, studies have shown that they are not more effective than spinal morphine and that there are probably no advantages in giving them routinely to women already receiving a morphine-containing spinal anesthetic.44–51 One study also reported the same lack of efficacy when morphine had been administered epidurally.52 Reasons for this are that the analgesic effect of a single-shot TAP block does not last as long as the analgesia provided by a spinal dose of morphine and that uterine cramping is not relieved by a TAP block. It has therefore been suggested that TAP blocks should only be offered to selected women who cannot, or did not, receive spinal morphine or to those experiencing severe breakthrough pain despite multimodal analgesia,53–57 particularly if abdominal wall pain is the dominant feature of the severe pain. Other studies on TAP block have confirmed its limited role in postoperative analgesia when spinal anaesthesia with a long acting opioid such as morphine is used as well as the use of TAP block for cesarean delivery under general anesthesia.58–60 The benefit of adding antihyperalgesic adjuvants (i.e. clonidine) to TAP solutions remains to be further studied.61 Threading bilateral catheters into the TAP for repeated boluses every 8 hours have been shown to provide successful analgesia for up to 72 hours after delivery.62 Of note, local anesthetic toxicity has been reported within 30 minutes of injection,63–65 and it is therefore important to adjust the local anesthetic dosing to women’s weight, to monitor for possible signs of systemic toxicity, and to be prepared to manage seizures.
The Quadratus Lumborum block (QLB) has also been used for postoperative analgesia after cesarean delivery. The main advantage of QLB compared to the TAP block is the extension of local anesthetic agent beyond the transversus abdominis plane to the thoracic paravertebral space. Two studies on QLB for post-operative analgesia after caesarean section under spinal, have reported it significantly reduces morphine consumption in combination with a multimodal analgesic regimen. 66, 67
In summary, severe acute pain after cesarean delivery despite multimodal analgesia is not uncommon and requires early identification and management of severe pain to prevent persistent pain, surgery-related symptoms with neuropathic characteristics, and the very rare case of chronic postcesarean pain. In women with risk factors for postoperative pain or with allergies precluding the use of morphine and/or NSAIDs, additional modalities should be offered. In the future, more studies to identify preoperatively who may be at risk for pain are likely to propose tailored postcesarean analgesia.68
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