Stanley Salmons

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Stanley Salmons
Stanley Salmons.jpg
Professor Stanley Salmons in 2012
Born
Stanley Salmons

April 14 1939
Lower Clapton, east London
SpousePaula Salmons

Stanley Salmons (born 1939) is a British academic and scientist. A Professor Emeritus of Medical Cell Biology at Liverpool University, [1] he is known for his pioneering research in the neurology, biochemistry and physiology of skeletal muscle. [2] [3] In 1967 he designed the first implantable neuromuscular stimulator and in 1969 he "was the first to introduce the design of the buckle-type transducer for recording directly in vivo tendon forces in animals." [4] His 1976 work with the implanted electrical "pacemakers" on rabbit muscles (published in Nature ) clarified the relationship between nerve signals and muscle chemistry and established the adaptive nature of skeletal muscle. [5] The associated changes in myosin isoforms overturned the accepted notion that a terminally differentiated tissue was incapable of re-expressing its genome.

Contents

Life and career

Salmons was born in Lower Clapton, east London, and was educated at St. Marylebone Grammar School. He was awarded a Royal Scholarship to attend the Imperial College in London, from which he graduated in physics and went on to gain a D.I.C. in Electronics and Communications. Salmons later attended the University College London on a Nuffield Foundation bursary, where he graduated with a master's degree in physiology. He was then appointed to a research fellowship in the Department of Anatomy, University of Birmingham, where he subsequently held a Stothert Research Fellowship of the Royal Society. He also worked for a time in the Department of Physiology at Harvard Medical School.

He was a senior lecturer when he left Birmingham University for the University of Liverpool, where he was professor of medical cell biology from 1987 until 1996 and is now a professor emeritus. [6] Salmons gave the 1989 Erasmus Wilson Demonstration at the Royal College of Surgeons of England, [7] and has also served as Director of the British Heart Foundation Skeletal Muscle Assist Research Group. He is a fellow of the Institute of Physics and Engineering in Medicine and of the Anatomical Society and was a former president of the International Society on Biotelemetry. He helped found the International Functional Electrical Stimulation Society and is an honorary member of the board of directors for Deutsche Gesellschaft für Elektrostimulation und Elektrotherapie. [8]

Salmons has written over 200 scientific articles and 12 scientific books, as well as more than 40 short stories, 19 novels, and 2 children's books. [9] [10]

Bibliography (selective)

Fiction

Most cited peer-reviewed articles

Related Research Articles

<span class="mw-page-title-main">Motor neuron</span> Nerve cell sending impulse to muscle

A motor neuron is a neuron whose cell body is located in the motor cortex, brainstem or the spinal cord, and whose axon (fiber) projects to the spinal cord or outside of the spinal cord to directly or indirectly control effector organs, mainly muscles and glands. There are two types of motor neuron – upper motor neurons and lower motor neurons. Axons from upper motor neurons synapse onto interneurons in the spinal cord and occasionally directly onto lower motor neurons. The axons from the lower motor neurons are efferent nerve fibers that carry signals from the spinal cord to the effectors. Types of lower motor neurons are alpha motor neurons, beta motor neurons, and gamma motor neurons.

The muscular system is an organ system consisting of skeletal, smooth, and cardiac muscle. It permits movement of the body, maintains posture, and circulates blood throughout the body. The muscular systems in vertebrates are controlled through the nervous system although some muscles can be completely autonomous. Together with the skeletal system in the human, it forms the musculoskeletal system, which is responsible for the movement of the body.

<span class="mw-page-title-main">Smooth muscle</span> Involuntary non-striated muscle

Smoothmuscle is one of the three major types of vertebrate muscle tissue, the others being skeletal and cardiac muscle. It can also be found in invertebrates and is controlled by the autonomic nervous system. It is non-striated, so-called because it has no sarcomeres and therefore no striations. It can be divided into two subgroups, single-unit and multi-unit smooth muscle. Within single-unit muscle, the whole bundle or sheet of smooth muscle cells contracts as a syncytium.

<span class="mw-page-title-main">Skeletal muscle</span> One of three major types of muscle

Skeletal muscle is one of the three types of vertebrate muscle tissue, the other being cardiac muscle and smooth muscle. They are part of the voluntary muscular system and typically are attached by tendons to bones of a skeleton. The skeletal muscle cells are much longer than in the other types of muscle tissue, and are also known as muscle fibers. The tissue of a skeletal muscle is striated – having a striped appearance due to the arrangement of the sarcomeres.

<span class="mw-page-title-main">Sarcomere</span> Repeating unit of a myofibril in a muscle cell

A sarcomere is the smallest functional unit of striated muscle tissue. It is the repeating unit between two Z-lines. Skeletal muscles are composed of tubular muscle cells which are formed during embryonic myogenesis. Muscle fibers contain numerous tubular myofibrils. Myofibrils are composed of repeating sections of sarcomeres, which appear under the microscope as alternating dark and light bands. Sarcomeres are composed of long, fibrous proteins as filaments that slide past each other when a muscle contracts or relaxes. The costamere is a different component that connects the sarcomere to the sarcolemma.

In biology, a motor unit is made up of a motor neuron and all of the skeletal muscle fibers innervated by the neuron's axon terminals, including the neuromuscular junctions between the neuron and the fibres. Groups of motor units often work together as a motor pool to coordinate the contractions of a single muscle. The concept was proposed by Charles Scott Sherrington.

Weakness is a symptom of many different medical conditions. The causes are many and can be divided into conditions that have true or perceived muscle weakness. True muscle weakness is a primary symptom of a variety of skeletal muscle diseases, including muscular dystrophy and inflammatory myopathy. It occurs in neuromuscular junction disorders, such as myasthenia gravis.

<span class="mw-page-title-main">Muscle cell</span> Type of cell found in muscle tissue

A muscle cell, also known as a myocyte, is a mature contractile cell in the muscle of an animal. In humans and other vertebrates there are three types: skeletal, smooth, and cardiac (cardiomyocytes). A skeletal muscle cell is long and threadlike with many nuclei and is called a muscle fiber. Muscle cells develop from embryonic precursor cells called myoblasts.

<span class="mw-page-title-main">Cardiac conduction system</span> Aspect of heart function

The cardiac conduction system transmits the signals generated by the sinoatrial node – the heart's pacemaker, to cause the heart muscle to contract, and pump blood through the body's circulatory system. The pacemaking signal travels through the right atrium to the atrioventricular node, along the bundle of His, and through the bundle branches to Purkinje fibers in the walls of the ventricles. The Purkinje fibers transmit the signals more rapidly to stimulate contraction of the ventricles.

<span class="mw-page-title-main">Neuromuscular junction</span> Junction between the axon of a motor neuron and a muscle fiber

A neuromuscular junction is a chemical synapse between a motor neuron and a muscle fiber.

<span class="mw-page-title-main">Functional electrical stimulation</span> Technique that uses low-energy electrical pulses

Functional electrical stimulation (FES) is a technique that uses low-energy electrical pulses to artificially generate body movements in individuals who have been paralyzed due to injury to the central nervous system. More specifically, FES can be used to generate muscle contraction in otherwise paralyzed limbs to produce functions such as grasping, walking, bladder voiding and standing. This technology was originally used to develop neuroprostheses that were implemented to permanently substitute impaired functions in individuals with spinal cord injury (SCI), head injury, stroke and other neurological disorders. In other words, a person would use the device each time he or she wanted to generate a desired function. FES is sometimes also referred to as neuromuscular electrical stimulation (NMES).

<span class="mw-page-title-main">Muscle contraction</span> Activation of tension-generating sites in muscle

Muscle contraction is the activation of tension-generating sites within muscle cells. In physiology, muscle contraction does not necessarily mean muscle shortening because muscle tension can be produced without changes in muscle length, such as when holding something heavy in the same position. The termination of muscle contraction is followed by muscle relaxation, which is a return of the muscle fibers to their low tension-generating state.

<span class="mw-page-title-main">End-plate potential</span> Voltages associated with muscle fibre

End plate potentials (EPPs) are the voltages which cause depolarization of skeletal muscle fibers caused by neurotransmitters binding to the postsynaptic membrane in the neuromuscular junction. They are called "end plates" because the postsynaptic terminals of muscle fibers have a large, saucer-like appearance. When an action potential reaches the axon terminal of a motor neuron, vesicles carrying neurotransmitters are exocytosed and the contents are released into the neuromuscular junction. These neurotransmitters bind to receptors on the postsynaptic membrane and lead to its depolarization. In the absence of an action potential, acetylcholine vesicles spontaneously leak into the neuromuscular junction and cause very small depolarizations in the postsynaptic membrane. This small response (~0.4mV) is called a miniature end plate potential (MEPP) and is generated by one acetylcholine-containing vesicle. It represents the smallest possible depolarization which can be induced in a muscle.

Muscle weakness is a lack of muscle strength. Its causes are many and can be divided into conditions that have either true or perceived muscle weakness. True muscle weakness is a primary symptom of a variety of skeletal muscle diseases, including muscular dystrophy and inflammatory myopathy. It occurs in neuromuscular junction disorders, such as myasthenia gravis. Muscle weakness can also be caused by low levels of potassium and other electrolytes within muscle cells. It can be temporary or long-lasting. The term myasthenia is from my- from Greek μυο meaning "muscle" + -asthenia ἀσθένεια meaning "weakness".

<span class="mw-page-title-main">Myofilament</span> The two protein filaments of myofibrils in muscle cells

Myofilaments are the three protein filaments of myofibrils in muscle cells. The main proteins involved are myosin, actin, and titin. Myosin and actin are the contractile proteins and titin is an elastic protein. The myofilaments act together in muscle contraction, and in order of size are a thick one of mostly myosin, a thin one of mostly actin, and a very thin one of mostly titin.

Electrical muscle stimulation (EMS), also known as neuromuscular electrical stimulation (NMES) or electromyostimulation, is the elicitation of muscle contraction using electric impulses. EMS has received an increasing amount of attention in the last few years for many reasons: it can be utilized as a strength training tool for healthy subjects and athletes; it could be used as a rehabilitation and preventive tool for people who are partially or totally immobilized; it could be utilized as a testing tool for evaluating the neural and/or muscular function in vivo. EMS has been proven to be more beneficial before exercise and activity due to early muscle activation. Recent studies have found that electrostimulation has been proven to be ineffective during post exercise recovery and can even lead to an increase in Delayed onset muscle soreness (DOMS).

Jozef Cywinski is a Polish-American scientist, a specialist in the field of biomedical engineering and specifically in electrical stimulation of living organisms. His work has been the subject of 12 patents, two books and over 100 scientific publications. He developed several first-on-the-market electro-medical devices like cardiac stimulators pacemakers, train-of-four nerve stimulators, PACS, EMS, TENS and Veinoplus calf pump stimulators.

Ludwig Julius Budge was a German physiologist.

<span class="mw-page-title-main">Sliding filament theory</span> Explanation of muscle contraction

The sliding filament theory explains the mechanism of muscle contraction based on muscle proteins that slide past each other to generate movement. According to the sliding filament theory, the myosin of muscle fibers slide past the actin during muscle contraction, while the two groups of filaments remain at relatively constant length.

<span class="mw-page-title-main">Paul Hunter Peckham</span> American academic

Paul Hunter Peckham is a professor of biomedical engineering and orthopedics at the Case Western Reserve University, and holds eight patents related to neural prosthetics. Peckham's research involves developing prostheses to restore function in the upper extremities for paralyzed individuals with spinal cord injury.

References

  1. University of Liverpool. Emeritus Professors. Retrieved 17 December 2012.
  2. Preedy, Victor R. and Peters, Timothy J.(2002). Skeletal Muscle: Pathology, Diagnosis and Management of Disease, p. 555. Cambridge University Press.
  3. Troidl, Hans et al. (1998). Surgical Research: Basic Principles and Clinical Practice, p. 10. Springer.
  4. Komi, Paavo V. (2011). Neuromuscular Aspects of Sports Performance. John Wiley & Sons.
  5. "Nerve Signals Dictate Muscle Chemistry". New Scientist, p 93. 14 October 1976. Retrieved 17 December 2012.
  6. Anapol, Fred; German, Rebecca Z.;Jablonski, Nina G. (eds.) (2004). Shaping Primate Evolution: Form, Function, and Behavior, p. 227. Cambridge University Press. ISBN   0521811074
  7. BMJ (April 1989). PMC   1836372 Notes, Vol 298, p. 1190.
  8. Krames, Elliot (2009). Neuromodulation. Academic Press. p. 59. ISBN   978-0123742483.
  9. Krieger, Candace. "Stanley Salmons turns his microscope on fiction-writing". Jewish Chronicle. Retrieved 17 December 2012.
  10. Biotelemetry XIV. Tectum Verlag. 1998. pp. 243–250. ISBN   3828890121.
  11. 1 2 "Google Scholar".
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