This is a story that was published on BBC website in 2009. Around the world millions of children are not getting a proper education because their families are too poor to afford to send them to school. In India, one schoolboy is trying to change that.
![]() REGIONAL ANAESTHESIA AND TOURNIQUET PAIN CONTROVERSY I still see people questioning about tourniquet pain and " how can patient have tourniquet pain when I have given the perfect block" There are some misconceptions, rather misunderstandings about Tourniquet Pain and today I would like to clear this simple controversy. 1st of all, everyone is right about Tourniquet Pain (TP), so what is the controversy? Controversy is about the understanding of this Pain. TP is unavoidable, we have to understand the TWO TYPES; TPP and TIP i.e Tourniquet Pressure Pain and Tourniquet Ischaemic Pain. I created this classification to clear this controversy. TOURNIOUET PRESSURE PAIN (TPP) or EARLY TOURNIQUET PAIN This pain is from HIGH PRESSURE that is applied to the limb (100mmHg above systolic pressure) to prevent arterial bleed and hence the name ARTERIAL TOURNIQUET. This pain is simple pain that is noticed by everyone when the Blood Pressure Cuff goes up during measurement of Blood Pressure, many patient feel very uncomfortable with this (observe the expression on patient’s face when the NIBP goes up for the 1st time esp in those with High BP). This is what we call TPP and this is NOT SEEN in patients under GA, you need to be awake to feel this pain. This pain originates from the cutaneous tissues and transmitted through Aδ fibres ( these get blocked by Tourniquet Pressure itself later, see under TIP). So in patients who are going to be awake it is important to block these fibres. For e.g. in forearm surgery with tourniquet under any type of Brachial Plexus block, it is important to block the Intercostobrachial nerve as it originates from T2 and is not blocked with any of the approaches to the brachial plexus. TOURNIOUET ISCHAEMIC PAIN (TIP) This is the pain that can not be blocked by even the BEST Nerve/ Plexus Block. TIP can be observed even under GA or in patients undergoing surgery under SAB or Epidural Anaesthesia. Inflation of a tourniquet is followed by the development of a dull aching pain after 30-60 minutes. This manifests as an increase in heart rate (HR)/ Respiratory Rate (RR) and blood pressure ( BP) in patients under general anaesthesia (RR changes are often more evident than HR changes in patients breathing Spontaneously) . The mechanism as to how such pain arises is thought to be due to selective pain transmission of unmyelinated, slowly conducting C fibres (0.5 – 2.0 m/sec as compared to 12-30 m/sec in A δ fibres). These fibres are continuously stimulated by skin compression, with loss of inhibition at the dorsal horn by larger myelinated Aδ fibres. With prolonged application, the conduction in larger myelinated fibres (Aδ) is inhibited by mechanical compression by the tourniquet (basis for Tourniquet Anaesthesia). Tourniquet pain, which occurs under apparently adequate neuraxial anaesthesia, is thought to occur as C fibres are more resistant to local anaesthetic conduction block. Also, with time, as the level of the block and concentration of anaesthesia decreases, C fibres regain function faster than A fibres. REDUCING TOURNIQUET PAIN Various methods have been tried to decrease the incidence of tourniquet pain, but none are completely satisfactory, except tourniquet deflation. Techniques used include: • The addition of Opioids like Morphine, or clonidine, to the neuraxial block. The addition of morphine delays the onset of pain. • Intravenous (IV) Ketamine 0.1 mg/kg. The N-methyl d-aspartate (NMDA) antagonist decreases central sensitisation of C fibre stimulation. • Preoperative Gabapentin. • IV/oral Clonidine. It may cause increased blood pressure drop after tourniquet release. • Circumferential subcutaneous infiltration of local anaesthetic or application of EMLA Cream • Wider cuff with lower inflation pressure. TOURNIQUET AND LIMB ISCHEMIA Upper limit for the duration of inflation: 30 mins - 4 hours At 30 min, onset of Anaerobic Metabolism starts > 1 hour of ischaemia – Electron Microscopy shows depletion of glycogen granules in the sarcoplasm of muscle fibres At 2 hours: Lesions associated with Acidosis are seen in the muscles – Mitochondrial swelling – Myelin degeneration – Z-line lysis Most of these changes are usually reversible with reperfusion. Reperfusion injuries is another topic on its own. CONCLUSIONS: Tourniquet pain is classified into early TPP and late TIP. Nerve blocks or cutaneous infiltration will prevent TPP but not late Ischemic pain i.e TIP. Additives can help in prolonging the onset of TIP. α Agonist as additives or as infusion are helpful in prolonging the onset of TIP but the use of IV Opioids is disappointing ( effect is transient and only helps in treating the numbers on the monitor) PRONE POSITION: PERI-OP VISUAL LOSS (POLV), ION, CRAO, CRVO AND INDUCED HYPOTENSION
Visual loss after spinal fusion surgery is a rare but devastating complication with a reported incidence of 0.017 to 0.1 percent. The major causes of visual loss in this patient population include 1. Ischemic Optic Neuropathy (ION) 2. Central Retinal Artery Occlusion (CRAO) and 3. Central Retinal Vein Occlusion (CRVO). POSITIONING AND CRAO and CRVO CRAO and CRVO are attributed to embolic load and/or direct globe compression, emphasizing the need to protect the eyes from direct pressure while in the prone position. ISCHEMIC OPTIC NEUROPATHY (ION)***** ION almost universally results in PERMANENT VISUAL LOSS. In 2012, the Postoperative Visual Loss (POVL) Study Group reported the findings of their multicenter case control study that used data from known ION cases registered in the American Society of Anesthesiologists POVL Registry and control cases from 17 United States academic medical centers. INDEPENDENT RISK FACTORS FOR THE DEVELOPMENT OF ION 1. Male sex 2. Obesity 3. Use of the Wilson frame (head lower than the heart) 4. Longer anaesthetic time 5. Greater estimated blood loss and 6. Lower percent of colloid in the nonblood fluid replacement Using these risk factors and the reported incidence of POVL from ION in the literature, the POVL Study Group created a risk prediction model that may help surgeons and anesthesia providers modify their care plans and define the risk of ION to patients . RISK MODIFICATION STRATEGIES FOR ION AFTER PRONE SPINE SURGERY 1. Positioning with the head level with or above the heart (Tilt The Whole Table) 2. Minimizing anaesthetic duration and blood loss ( Staged Procedure if necessary) 3. Use of both colloids and crystalloids for intravascular volume replacement 4. Monitoring hemoglobin periodically during cases with significant blood loss and 5. Optimization of hemodynamics with maintenance of blood pressure within 20 percent of baseline. Patients scheduled for historically lengthy (longer than four hours) spine surgery in the prone position should be informed of the small but increased risk of ION. When possible, staging of long procedures should be considered. CONTROLLED/ INDUCED HYPOTENSION The use of controlled hypotension is NOT recommended in patients undergoing spine surgery. Induced hypotension has historically been advocated as a mechanism to reduce blood loss during a variety of surgical procedures. WHY LOW BP DOES NOT REDUCE BLOOD LOSS Reduced wound blood flow as a result of lower arterial blood pressure has been the mechanism cited for reduction in blood loss. However, epidural venous plexus pressure and intraosseous pressure, both important determinants of blood loss in spine surgery, are independent of arterial blood pressure. INDUCED HYPOTENSION and SPINAL CORD ISCHEMIA The most important reason to avoid the use of induced hypotension is the potential for end-organ ischemia. In particular, patients with severe spinal stenosis are at risk for SPINAL CORD ISCHEMIA and should be maintained during anaesthesia at or near their usual blood pressure. In addition, spinal instrumentation and distraction can reduce SPINAL CORD PERFUSION AND RESULT IN ISCHEMIA. Therefore, adequate arterial blood pressure should be maintained during instrumented spinal surgery as one measure to avoid neurologic damage. INDUCED HYPOTENSION AND POVL As explained above, visual loss is a rare but potentially devastating postoperative complication of prone spinal surgery. Ischemic optic neuropathy (ION) is the most common cause of postoperative visual loss. Although the causes of ischemic optic neuropathy have not been fully elucidated, tissue edema with reduced perfusion of the optic nerve is a suggested etiology. ![]() “Most of the successful people I've known are the ones who do more listening than talking.” —Bernard Baruch One of the traits that makes one an excellent clinician is that they are good listeners. The doctor’s distinctive listening tool—the stethoscope. Many children have played game of doctor-doctor as a child and the most important toy in that game is the stethoscope. This year, 2016, marks the stethoscope’s 200th birthday. Invented by a French physician, René Laennec, in 1816 it is perhaps the true symbol of medicine. First used in a Paris hospital, the story goes that Dr. Laennec invented the stethoscope because he wasn’t comfortable putting his ear on the chest of a woman to hear her heart. Born in 1781 and raised by one uncle who was a priest and another uncle who was a medical school dean, Laennec was, like most doctors, a superior student. Although his lawyer-father tried to discourage him from a medical career, he would go on to become the father of clinical auscultation. According to a very good profile of this pioneering physician by the National Center for Biotechnology Information, Dr. Laennec “wrote the first descriptions of bronchiectasis and cirrhosis and also classified pulmonary conditions such as pneumonia, bronchiectasis, pleurisy, emphysema, pneumothorax, phthisis, and other lung diseases from the sounds he heard with his invention. He perfected the art of physical examination of the chest and introduced many clinical terms still used today.” In writing the classic 1819 treatise on his application of clinical auscultation, he offered: “I happened to recollect a simple and well-known fact in acoustics ... the great distinctness with which we hear the scratch of a pin at one end of a piece of wood on applying our ear to the other. Immediately, on this suggestion, I rolled a quire of paper into a kind of cylinder and applied one end of it to the region of the heart and the other to my ear, and was not a little surprised and pleased to find that I could thereby perceive the action of the heart in a manner much more clear and distinct than I had ever been able to do by the immediate application of my ear.” Dr. Laennec, who was also trained by Napoleon’s personal physician, died of tuberculosis in 1826 at age 45. According to the NCBI story, “during those last months, he asked his nephew to auscultate his chest and to describe what was heard. The findings were as alarming as they were familiar to this great chest physician who had heard the same sounds a thousand times before. By his own invention, he could no longer escape the ironic truth that he was dying from tuberculosis—the disease that he helped to elucidate and understand with his stethoscope would soon take his life.” With today’s amazing technological advances in medical care, one might think the stethoscope will become a relic of the past—an antique. For many doctors maybe that’s the case even today, but Stethoscope still hangs around the necks of all good physicians. It may have advanced with some modifications but the principles remain the same. Modified from a blog |
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