International Journal of Anesthesiology & Pain Medicine

Table 1: Demographic data.

As compared to the baseline, mean heart rate was increased in Group A at 1, 5, 10, 15, 20 and 30 minutes (Table 2). Maximum heart rate in-Group A was 89.30- ± 14.62 bpm at 5 minutes at 5 minute. In contrast, HR significantly decreased in Group N at 30, 40, 50 and 60 minutes with minimum mean HR was 65.40 ± 11.34 bpm. In-group N, 40% of the patient required atropine for the treatment of bradycardia, which was statistically significant (p=0.01) (Table 3).

Table 2: Comparison of mean HR with baseline in each group.

Table 3: Intra operative events.

As compared to baseline, MAP didn’t change significantly in Group A except at one minute (Table 3). However, in-group N, MAP significantly decreased all the times (Table 4) and treatment is required in 40% cases (Table 3).

Table 4: Comparison of mean MAP with baseline in each group.

Intragroup comparison, heart rate was significantly high in atropine group as compared to placebo group at 1, 5, 10 and 15 minutes. Whereas at 20, 40,50 and 60 minutes HR was significantly lower as compared to other groups in placebo group (Figure 1).

Figure 1: Intra group comparison of trend HR.

Intra group comparison, MAP was significantly high in atropine group as compared to placebo group at 1 minute. Whereas at 5, 10,15, 30, 40, 50, and 60 minute MAP was lower in placebo as compared to atropine (Figure 2).

Figure 2: Intra group comparison of trend MAP.

Intraoperatively, 60% patient developed hypotension (p=0.01) and 40% developed bradycardia (p=0.01) in placebo group who required treatment, which was statistically significant as compared to other group (Table 3). None of the patients in both group developed side effects like intra operative angina and intra/postoperative confusion till 6 h postoperatively. No other side effects were detected in any of the groups.

Discussion

The most common serious side effects from spinal anesthesia are hypotension and bradycardia and closed claims surveys of 40,000- 550,000 spinal anesthetics indicate an incidence of cardiac arrest from 0.04–1/10,000 [1,2,5,6]. Risk factors for hypotension block are height T5 or greater, age 40 yrs or greater, baseline systolic blood pressure less than 120 mmHg, and spinal puncture above L3–L4. Risk factors for development of bradycardia include baseline heart rate less than 60 bpm, ASA PS I, use of β-adrenergic blockers, prolonged PR interval on electrocardiogram, and block height T5 or greater [1,7].

Currently various techniques are been using for the prevention of hypotension and bradycardia which include pre or co-loading of IV fluid, vasopressors, and physical methods such as table tilt, leg binders, and compression devices [8-14]. However, a Cochrane review concluded that none of these techniques alone is effective and suggested that the future research be directed towards a combination of interventions [11]. This study aimed to prevent the spinal anesthesia induced hypotension with combination of preloading with normal saline 10 ml/kg and pretreatment with either IV atropine.

Atropine is esters of an aromatic acid combined with an organic base. It competitively blocks acetylcholine binding to its receptor and prevents receptor activation thus cellular effects of acetylcholine are inhibited. In general, atropine lowers the parasympathetic activity of all muscles and glands regulated by the parasympathetic nervous system and increase heart rate via abolishing the vagal tone acting on M2 receptor at heart.

The present study showed that the incidence of bradycardia was significantly high at various time (Table 1) in placebo group and require treatment with atropine (p=0.01) compared to atropine groups. Compared to baseline, heart rate was high in in atropine group at 5 minutes, which corresponds to the peak effect of the IV atropine. The increase in HR is statistically significant but only one patient required treatment for tachycardia. Similarly, MAP was also lower in placebo group at most of the time compared to atropine group. In present study, 60% patient in placebo group and 5% patient in atropine group required mephentermine for the treatment of hypotension. Use of mephentermine was significant (p=0.01) in placebo group as compared atropine group. This indicates that both incidence and severity of hypotension are greater in placebo group as compared to the atropine group. The findings are similar to various other studies. IV atropine after a crystalloid infusion in patients undergoing SA could increase HR very quickly in a dose-dependent manner and decrease the incidence of significant hypotension also in a dose-dependent manner [15]. PUN Nze demonstrated the incidence and severity of hypotension were reduced in parturients undergoing

section under spinal anesthesia with use of prophylactic intravenous bolus of atropine [16]. Thus intravenous atropine may be a useful supplement to the existing methods in preventing hypotension induced by spinal anaesthesia. However, when IM atropine was used, Hirabayashi et al. did not demonstrate any beneficial effect in hemodynamic stability during SA because the absorption of IM atropine may be unpredictable, and the onset may have been too slow in comparison to the onset of hypotension after SA [17]. Another anticholinergic agent, glycopyrrolate, when administered IV after SA increased HR and reduced the severity of hypotension in women presenting for elective cesarean section and concluded that glycopyrrolate reduce the severity of hypotension after SA, evidenced by reduced ephedrine requirements (p=0.002) [18]. Though, the present study didn’t show any significant side effect in intra/ post-operative period (Table 3) many practitioners hesitate to administer atropine as it cross blood brain barrier and concerned about the central CNS effects of atropine. Glycopyrrolate may have similar effect in preventing spinal induced hypotension and bradycardia but it cannot be concluded from present study and further investigation is required. All patients were observed for 6 h in postoperative ward for the study and no untoward effects were noted.

In summary, hypotension and bradycardia after induction of spinal anesthesia were common in elderly patients. The use of IV atropine one minute after the induction of spinal anesthesia in elderly patient was beneficial in maintaining hemodynamic stability. Although, the incidence of tachycardia was high in atropine group the incidence of clinically significant tachycardia (HR>140 bpm) were comparable among all the three groups. None of the patients in both groups developed other side effects. So, the study suggests prophylactic IV atropine can be safely used in elderly patient for the prevention of spinal anesthesia induced hypotension.

Limitations

Amount of blood loss, which can influence the hemodynamic parameters, was not recorded in our study. For the measurement of blood pressure oscillatory noninvasive blood pressure methods was used, invasive blood pressure monitoring method would have been used to monitor real time blood pressure. Only urological surgeries (TURP, CA UB) were taken for the study, which require only lower thoracic block for surgery. This population may not be the actual representative of the SA induced hypotension associated with higher blocks more than T8.

Conclusions

The use of prophylactic IV atropine after one minute of induction of spinal anesthesia reduces the incidence and severity of the spinal anesthesia induced hypotension as well as the incidence of bradycardia in elderly patients. The need of vasopressors also decreases significantly.

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