Friday, January 6, 2012

Destiny of the Republic

Destiny of the Republic: A Tale of Madness, Medicine and the Murder of a President, by Candice Millard, superimposed on Intermediate Physics for Medicine and Biology.
Destiny of the Republic:
A Tale of Madness, Medicine
and the Murder of a President,
by Candice Millard.

Regular readers of this blog know that I am in the habit of listening to audio books while I take my dog Suki on her daily walks. My tastes lean toward science, history, and biography, and I always keep a watch out for biological or medical physics in these books. Over the Christmas break, I listened to Destiny of the Republic: A Tale of Madness, Medicine and the Murder of a President, by Candice Millard, about the assassination of President James Garfield in 1881, shot by madman Charles Guiteau.

The book tells the fascinating story of Garfield’s nomination at the Republican National Convention in 1880, back in a time when conventions were less choreographed and predictable than they are today. Garfield nominated his fellow Ohioan John Sherman (General William Tecumseh Sherman’s brother), who was running against Senator James Blaine and former president Grant. After many ballots in which no nominee obtained a majority, the delegates turned to Garfield as their compromise choice. After being chosen the Republican nominee, he defeated Democrat and former Civil War general Winfield Scott Hancock in the general election.

A few months after being sworn in, Garfield was shot by Guiteau, who had applied for a job in the new administration but had been turned down. The bullet did not kill Garfield immediately, and he lingered on for weeks. At this point, medical physics enters the story through one of the book’s subplots about the career of Alexander Graham Bell, inventor of the telephone. Millard tells the tale of how Bell set up one of his early telephones for demonstration at the 1876 Centennial Exposition, but was ignored until a chance meeting with his acquaintance, Emperor Pedro II of Brazil, who drew attention to Bell’s display. Upon hearing that the President had been shot, Bell quickly invented a metal detector with the goal of locating the bullet still lodged in Garfield’s abdomen. The detector is based on the principle of electromagnetic induction, discussed in Section 8.6 of the 4th edition of Intermediate Physics for Medicine and Biology. A changing magnetic field induces eddy currents in a nearby conductor. These eddy currents produce their own magnetic field, which is then detected. Essentially, the device monitored changes in the inductance of the metal detector caused by the bullet. Such metal detectors are now common, particularly for nonmedical uses such as searching for metal objects buried shallowly in the ground. At the time, the device was rather novel. Michael Faraday (and, independently, Joseph Henry) had discovered electromagnetic induction in 1831, and Maxwell’s equations summarizing electromagnetic theory were formulated by James Maxwell in 1861, only twenty years before Garfield’s assassination. Being a champion of medical and biological physics, I wish I could say that Bell’s invention saved the president’s life, or at least had a positive effect during his treatment. Unfortunately, it did not, in part because of interference from metal springs in the mattress Garfield laid on, but mainly because the primary physician caring for Garfield, Dr. Willard Bliss, insisted that Bell only search the right side of the body where he believed the bullet was located, when in fact it was on the unexplored left side.

Another issue discussed in the book is the development of antiseptic methods in medicine, pioneered by Joseph Lister in the 1860s. Apparently the direct damage caused by the bullet was not life-threatening, and Millard suggests that if Garfield had received no treatment whatsoever for his wounds, he would have likely survived. Unfortunately, the doctors of that era, being skeptical or hostile to Lister’s new ideas, probed Garfield’s wound with various non-sterile instruments, including their fingers. Garfield died of an infection, possibly caused by these actions.

I enjoyed Millard’s book, and came away with a greater respect for President Garfield. Bell’s metal detector was used to locate bullets in injured soldiers throughout the rest of the 19th century, until X rays became the dominant method for finding foreign objects. It is an early example of the application of electricity and magnetism to medicine.

Listen to Candice Millard speak about her book.

 Candice Millard speaking about Destiny of the Republic.
https://www.youtube.com/embed/TmebtlLULpY

Friday, December 30, 2011

Wilhelm Roentgen

The medical use of X rays is one of the main topics discussed in the 4th edition of Intermediate Physics for Medicine and Biology. However, Russ Hobbie and I don’t say much about the discoverer of X rays, Wilhelm Roentgen (1845–1923). Let me be more precise: we never mention Roentgen at all, despite his winning the first ever Nobel Prize in Physics in 1901. We do refer to the unit bearing his name, but in an almost disparaging way:
Problem 8 The obsolete unit, the roentgen (R), is defined as 2.08 x 109 ion pairs produced in 0.001 293 g of dry air. (This is 1 cm3 of dry air at standard temperature and pressure.) Show that if the average energy required to produce an ion pair in air is 33.7 eV (an old value), then 1 R corresponds to an absorbed does of 8.69 x 10-3 Gy and that 1 R is equivalent to 2.58 x 10-4 C kg-1.
Asimov's Biographical Encyclopedia of Science and Technology, by Isaac Asimov, superimposed on Intermediate Physics for Medicine and BIology.
Asimov's Biographical Encyclopedia
of Science and Technology,
by Isaac Asimov.
Roentgen’s story is told in Asimov’s Biographical Encyclopedia of Science and Technology. (My daughter gave me a copy of this book for Christmas this year; Thanks, Kathy!)
…The great moment that lifted Roentgen out of mere competence and made him immortal came in the autumn of 1895 when he was head of the department of physics at the University of Wurzburg in Bavaria. He was working on cathode rays and repeating some of the experiments of Lenard and Crookes. He was particularly interested in the luminescence these rays set up in certain chemicals.

In order to observe the faint luminescence, he darkened the room and enclosed the cathode ray tube in thin black cardboard. On November 5, 1895, he set the enclosed cathode ray tube into action and a flash of light that did not come from the tube caught his eye. He looked up and quite a distance from the tube he noted that a sheet of paper coated with barium platinocyanide was glowing. It was one of the luminescent substances, but it was luminescing now even though the cathode rays, blocked off by the cardboard, could not possibly be reaching it.

He turned off the tube; the coated paper darkened. He turned it on again; it glowed. He walked into the next room with the coated paper, closed the door, and pulled down the blinds. The paper continued to glow while the tube was in operation…

For seven weeks he experimented furiously and then, finally, on December 28, 1895 [116 years ago this week], submitted his first paper, in which he not only announced the discovery but reported all the fundamental properties of X rays...

The first public lecture on the new phenomenon was given by Roentgen on January 23, 1896. When he had finished talking, he called for a volunteer, and Kolliker, almost eighty years old at the time, stepped up. An X-ray photograph was taken of this hand—which shows the bones in beautiful shape for an octogenarian. There was wild applause, and interest in X rays swept over Europe and America.
You can learn more about X rays in Chapter 15 (Interaction of Photons and Charged Particles with Matter) and Chapter 16 (Medical Use of X Rays) in Intermediate Physics for Medicine and Biology.

Friday, December 23, 2011

Poisson's Ratio

One of the many new problems that Russ Hobbie and I added to the 4th edition of Intermediate Physics for Medicine and Biology deals with Poisson’s ratio. From Chapter 1:
Problem 25 Figure 1.20, showing a rod subject to a force along its length, is a simplification. Actually, the cross-sectional area of the rod shrinks as the rod lengthens. Let the axial strain and stress be along the z axis. They are related to Eq. 1.25, sz = E εz. The lateral strains εx and εy are related to sz by sz = - (E/ν) εx = -(E/ν) εy, where ν is called the “Poisson’s ratio” of the material.
(a) Use the result of Problem 13 to relate E and ν to the fractional change in volume ΔV/V.
(b) The change in volume caused by hydrostatic pressure is the sum of the volume changes caused by axial stresses in all three directions. Relate Poisson’s ratio to the compressibility.
(c) What value of ν corresponds to an incompressible material?
(d) For an isotropic material, -1 ≤ ν ≤ 0.5. How would a material with negative ν behave?
Elliott et al. (2002) measured Poisson’s ratio for articular (joint) cartilage under tension and found 1 ν 2. This large value is possible because cartilage is anisotropic: Its properties depend on direction.
The citation is to a paper by Dawn Elliott, Daria Narmoneva and Lori Setton, “Direct Measurement of the Poisson’s Ratio of Human Patella Cartilage in Tension,” in the Journal of Biomechanical Engineering, Volume 124, Pages 223–228, 2002. (Apologies to Dr. Narmoneva, whose name was misspelled in our book. It is now corrected in the errata, available at the book website.)

As hinted at in our homework problem, a particularly fascinating type of material has negative Poisson’s ratio. Some foams expand laterally, rather than contract, when you stretch them; see Roderic Lakes, “Foam Structures with a Negative Poisson’s Ratio,” Science, Volume 235, Pages 1038–1040, 1987. A model for such a material is shown in this video. Lakes’ website contains much interesting information about Poisson’s ratio. For instance, cork has a Poisson’s ratio of nearly zero, making it ideal for stopping wine bottles.

Simeon Denis Poisson (1781–1840) was a French mathematician and physicist whose name appears several times in Intermediate Physics for Medicine and Biology. Besides Poisson’s ratio, in Chapter 9 Russ and I present the Poisson equation in electrostatics, and its extension the Poisson-Boltzmann equation governing the electric field in salt water. Appendix J reviews the Poisson probability distribution. Finally, Poisson appeared in this blog before, albeit as something of a scientific villain, in the story of Poisson’s spot. Poisson is one of the 72 names appearing on the Eiffel Tower.

Friday, December 16, 2011

Gadolinium

While school children know the most famous elements listed in the periodic table (for example hydrogen, oxygen, and carbon), even many scientists are unfamiliar with those rare earth elements at the bottom of the table, listed under the generic label of lanthanides. But one of these, gadolinium (Gd, element 64), has become crucial for modern medicine because of its use as a contrast agent during magnetic resonance imaging. In Chapter 18 of the 4th edition of Intermediate Physics for Medicine and Biology, Russ Hobbie and I discuss gadolinium.
Differences in relaxation time are easily detected in an image. Different tissues have different relaxation times. A contrast agent containing gadolinium (Gd3+), which is strongly paramagnetic, is often used in magnetic resonance imaging. It is combined with many of the same pharmaceuticals used with 99mTc, and it reduces the relaxation time of nearby nuclei.
In 1999, Peter Caravan and his coworkers published a major review article about the uses of gadolinium in imaging, which has been cited over 1500 times (“Gadolinium(III) Chelates as MRI Contrast Agents: Structure, Dynamics, and Applications,” Chemical Reviews, Volume 99, Pages 2293–2352). The review is well written, and I reproduce the introduction below.
Gadolinium, an obscure lanthanide element buried in the middle of the periodic table, has in the course of a decade become commonplace in medical diagnostics.
Like platinum in cancer therapeutics and technetium in cardiac scanning, the unique magnetic properties of the gadolinium(III) ion placed it right in the middle of a revolutionary development in medicine: magnetic resonance imaging (MRI). While
it is odd enough to place patients in large superconducting magnets and noisily pulse water protons in their tissues with radio waves, it is odder still to inject into their veins a gram of this potentially toxic metal ion which swiftly floats among the water molecules, tickling them magnetically.

The successful penetration of gadolinium(III) chelates into radiologic practice and medicine as a whole can be measured in many ways. Since the approval of [Gd(DTPA)(H2O)]2- in 1988, it can be estimated that over 30 metric tons of gadolinium have been administered to millions of patients worldwide. Currently, approximately 30% of MRI exams include the use of contrast agents, and this is projected to increase as new agents and applications arise; Table 1 lists agents currently approved or in clinical trials. In the rushed world of modern medicine, radiologists, technicians, and nurses often refrain from calling the agents by their brand names, preferring instead the affectionate “gado.” They trust this clear, odorless 'magnetic light', one of the safest class of drugs ever developed. Aside from the cost ($50–80/bottle), asking the nurse to “Give him some gado” is as easy as starting a saline drip or obtaining a blood sample.

Gadolinium is also finding a place in medical research. When one of us reviewed the field in its infancy, in 1987, only 39 papers could be found for that year in a Medline search for “gado-” and MRI. Ten years later over 600 references appear each year. And as MRI becomes relied upon by different specialties, “gado” is becoming known by neurologists, cardiologists, urologists, opthamologists, and others in search of new ways to visualize functional changes in the body.

While other types of MRI contrast agents have been approved, namely an iron particle-based agent and a manganese(II) chelate, gadolinium(III) remains the dominant starting material. The reasons for this include the direction of MRI development and the nature of Gd chelates.
In Section 18.12 about Functional MRI, Russ and I again mention gadolinium.
Magnetic resonance imaging provides excellent structural information. Various contrast agents can provide information about physiologic function. For example, various contrast agents containing gadolinium are injected intravenously. They leak through a damaged blood-tissue barrier and accumulate in the damaged region. At small concentrations T1 is shortened.
Here at Oakland University, several of our Biomedical Sciences: Medical Physics PhD students study brain injury using this method. See, for instance, the dissertation Magnetic Resonance Imaging Investigations of Ischemic Stroke, Intracerebral Hemorrhage and Blood-Brain Barrier Pathology by Kishor Karki, 2009.

Friday, December 9, 2011

The Cyclotron

The 4th edition of Intermediate Physics for Medicine and Biology has its own Facebook group, and any readers of this blog who use Facebook are welcome to join. One nice feature of Facebook is that is encourages comments, such as the recent one that asked “Why isn’t there a chapter or a subchapter in the textbook ‘Intermediate physics for medicine and biology’ that refers to the fundamental concepts of the cyclotron and the betatron and how are they used in medicine?” This is a good question, because undoubtedly cyclotrons are important in nuclear medicine. I can’t do anything to change the 4th edition of our book, but this blog provides an opportunity to address such comments, and to try out possible text for a 5th edition.

Although the term does not appear in the index (oops…), the cyclotron is mentioned in Intermediate Physics for Medicine and Biology at the end of Section 17.9 (Radiopharmaceuticals and Tracers).
Other common isotopes are 201Tl, 67Ga, and 123I. Thallium, produced in a cyclotron, is chemically similar to potassium and is used in heart studies, though it is being replaced by 99mTc-sestamibi and 99mTc-tetrofosmin. Gallium is used to image infections and tumors. Iodine is also produced in a cyclotron and is used for thyroid studies.
Cyclotrons are again mentioned in Section 17.14 (Positron Emission Tomography)
Positron emitters are short-lived, and it is necessary to have a cyclotron for producing them in or near the hospital. This is proving to be less of a problem than initially imagined. Commercial cyclotron facilities deliver isotopes to a number of nearby hospitals. Patterson and Mosley (2005) found that 97% of the people in the United States live within 75 miles of a clinical PET facility.
(Note: on page 513 of our book, we omitted the word “emission” from the phrase “positron emission tomography” in the title of the Patterson and Mosley paper; again, oops…)

Perhaps the best place in Intermediate Physics for Medicine and Biology to discuss cyclotrons would be after Section 8.1 (The Magnetic Force on a Moving Charge). Below is some sample text that serves as a brief introduction to cyclotrons.
8.1 ½ The Cyclotron

One important application of magnetic forces in medicine is the cyclotron. Many hospitals have a cyclotron for the production of radiopharmaceuticals, or for the generation of positron emitting nuclei for use in Positron Emission Tomography (PET) imaging (see Chapter 17).

Consider a particle of charge q and mass m, moving with speed v in a direction perpendicular to a magnetic field B. The magnetic force will bend the path of the particle into a circle. Newton’s second law states that the mass times the centripetal acceleration, v2/r, is equal to the magnetic force

m v2/r = q v B . (8.4a)

The speed is equal to circumference of the circle, 2 π r, divided by the period of the orbit, T. Substituting this expression for v into Eq. 8.4a and simplifying, we find

T = 2 π m/(q B) . (8.4b)

In a cyclotron particles orbit at the cyclotron frequency, f = 1/T. Because the magnetic force is perpendicular to the motion, it does not increase the particles’ speed or energy. To do that, the particles are subjected periodically to an electric field that must change direction with the cyclotron frequency so that it is always accelerating, and not decelerating, the particles. This would be difficult if not for the fortuitous disappearance of both v and r from Eq. 8.4b, so that the cyclotron frequency only depends on the charge-to-mass ratio of the particles and the magnetic field, but not on their energy.

Typically, protons are accelerated in a magnetic field of about 1 T, resulting in a cyclotron frequency of approximately 15 MHz. Each orbit raises the potential of the proton by about 100 kV, and it must circulate enough times to raise its total energy to at least 10 MeV so that it can overcome the electrostatic repulsion of the target nucleus and cause nuclear reactions. For example, the high-energy protons may be incident on a target of 18O (a rare but stable isotope of oxygen), initiating a nuclear reaction that results in the production of 18F, an important positron emitter used in PET studies.
Since Intermediate Physics for Medicine and Biology is not a history book, I didn’t mention the interesting history of the cyclotron, which was invented by Ernest Lawrence in the early 1930s, for which he received the Nobel Prize in Physics in 1939. The American Institute of Physics Center for the History of Physics has a nice website about Lawrence’s invention. The same story is told, perhaps more elegantly, in Richard Rhodes masterpiece The Making of the Atomic Bomb (see Chapter 6, Machines). Lawrence played a major role in the Manhattan Project, using modified cyclotrons as massive mass spectrometers to separate the fissile uranium isotope 235U from the more abundant 238U.

Finally, I think it’s appropriate that Intermediate Physics for Medicine and Biology should have a section about the cyclotron, because my coauthor Russ Hobbie (who was the sole author of the first three editions of the textbook) obtained his PhD while working at the Harvard cyclotron. Thus, an unbroken path leads from Ernest Lawrence and the cyclotron to the publication of our book and the writing of this blog.

Friday, December 2, 2011

Feedback Loops

Negative feedback is an important concept in physiology. Russ Hobbie and I discuss feedback loops in Chapter 10 of the 4th edition of Intermediate Physics for Medicine and Biology. In the text and homework problems, we discuss several examples of negative feedback, including the regulation of breathing rate by the concentration of carbon dioxide in the alveoli, the prevention of overheating of the body by sweating, and the control of blood glucose levels by insulin. You can never have enough of these examples. Therefore, here is another homework problem related to negative feedback: regulation of blood osmolarity by antidiuretic hormone. Warning: the model is greatly simplified. It should be correct qualitatively, but not accurate quantitatively.
Section 10.3

Problem 15 ½ The osmolarity of plasma (C, in mosmole) is regulated by the concentration of antidiuretic hormone (ADH, in pg/ml, also known as vasopressin). As antidiuretic hormone increases, the kidney reabsorbs more water and the plasma osmolarity decreases, C=700/ADH. When osmoreceptors in the hypothalamus detect an increase of plasma osmolarity, they stimulate the pituitary gland to produce more antidiuretic hormone, ADH = C-280 for C greater than 280, and zero otherwise.
(a) Draw a block diagram of the feedback loop, including accurate plots of the two relationships.
(b) Calculate the operating point and the open loop gain (you may need to use four to six significant figures to determine the operating point accurately).
(c) Suppose the behavior of the kidney changed so now C=750/ADH. First determine the new value of C if the regulation of ADH is not functioning (ADH is equal to that found in part b), and then determine the value of C taking regulation of ADH by the hypothalamus into account.
You should find that this feedback loop is very effective at holding the blood osmolarity constant. For more about osmotic effects, see Chapter 5 of Intermediate Physics for Medicine and Biology.

Textbook of Medical Physiology, by Guyton and Hall, superimposed on Intermediate Physics for Medicine and Biology.
Textbook of Medical Physiology,
by Guyton and Hall.









Here is how Guyton and Hall describe the physiological details of this feedback loop in their Textbook of Medical Physiology (11th edition):
When osmolarity (plasma sodium concentration) increases above normal because of water deficit, for example, this feedback system operates as follows:

1. An increase in extracellular fluid osmolarity (which in practical terms means an increase in plasma sodium concentration) causes the special nerve cells called osmoreceptor cells, located in the anterior hypothalamus near the supraoptic nuclei, to shrink.

2. Shrinkage of the osmoreceptor cells casuse them to fire, sending nerve signals to additional nerve cells in the supraoptic nuclei, which then relay these signals down the stalk of the pituitary gland to the posterior pituitary.

3. These action potentials conducted to the posterior pituitary stimulate the release of ADH, which is stored in secretory granules (or vesicles) in the nerve endings.

4. ADH enters the blood stream and is transported to the kidneys, where it increases the water permeability of the late distal tubules, cortical collecting tubules, and the medullary collecting ducts.

5. The increased water permeability in the distal nephron segments causes increased water reabsorption and excretion of a small volume of concentrated urine.

Thus, water is conserved in the body while sodium and other solutes continue to be excreted in the urine. This causes dilution of the solutes in the extracellular fluid, thereby correcting the initial excessively concentrated extracellular fluid.
Feedback loops are central to physiology. Guyton and Hall write in their first introductory chapter
Thus, one can see how complex the feedback control systems of the body can be. A person’s life depends on all of them. Therefore, a major share of this text is devoted to discussing these life-giving mechanisms.

Friday, November 25, 2011

The Second Law of Thermodynamics

Russ Hobbie and I discuss thermodynamics in Chapter 3 of the 4th edition of Intermediate Physics for Medicine and Biology. We take a statistical perspective (similar to that used so effectively by Frederick Reif in Statistical Physics, which is Volume 5 of the Berkeley Physics Course), and discuss many topics such as heat, temperature, entropy, the Boltzmann factor, Gibbs free energy, and the chemical potential. But only at the very end of the chapter do we mention the central concept of thermodynamics: The second law.
In some cases, thermal energy can be converted into work. When gas in a cylinder is heated, it expands against a piston that does work. Energy can be supplied to an organism and it lives. To what extent can these processes, which apparently contradict the normal increase of entropy, be made to take place? The questions can be stated in a more basic form.

1. To what extent is it possible to convert internal energy distributed randomly over many molecules into energy that involves a change of a macroscopic parameter of the system? (How much work can be captured from the gas as it expands the piston?)

2. To what extent is it possible to convert a random mixture of simple molecules into complex and highly organized macromolecules?

Both these questions can be reformulated: under what conditions can the entropy of a system be made to decrease?

The answer is that the entropy of a system can be made to decrease if, and only if, it is in contact with one or more auxiliary systems that experience at least a compensating increase in entropy. Then the total entropy remains the same or increases. This is one form of the second law of thermodynamics. For a fascinating discussion of the second law, see Atkins (1994).
The Second Law:  Energy, Chaos, and Form,  by Peter Atkins, superimposed on Intermediate Physics for Medicine and Biology.
The Second Law:
Energy, Chaos, and Form,
by Peter Atkins.
The book by Peter Atkins, The Second Law, is published by the Scientific American Library, and is aimed at a general audience. It’s a wonderful book, and provides the best non-mathematical description of thermodynamics I know of. Atkins’ preface begins
No other part of science has contributed as much to the liberation of the human spirit as the Second Law of thermodynamics. Yet, at the same time, few other parts of science are held to be so recondite. Mention of the Second Law raises visions of lumbering steam engines, intricate mathematics, and infinitely incomprehensible entropy. Not many would pass C. P. Snow’s test of general literacy, in which not knowing the Second Law is equivalent to not having read a work of Shakespeare.

In this book I hope to go some way toward revealing the workings of the Law, and showing its span of application. I start with the steam engine, and the acute observations of the early scientists, and I end with a consideration of the processes of life. By looking under the classical formulation of the Law we see its mechanism. As soon as we do so, we realize how simple it is to comprehend, and how wide is its application. Indeed, the interpretation of the Second Law in terms of the behavior of molecules is not only straightforward (and in my opinion much easier to understand that the First Law, that of the conservation of energy), but also much more powerful. We shall see that the insight it provides lets us go well beyond the domain of classical thermodynamics, to understand all the processes that underlie the richness of the world.
Atkins’s book is at the level of a Scientific American article, with many useful (and colorful) pictures and historical anecdotes. The writing is excellent. For instance, consider this excerpt:
The Second Law recognizes that there is a fundamental dissymmetry in Nature…hot objects cool, but cool objects do not spontaneously become hot; a bouncing ball comes to rest, but a stationary ball does not spontaneously begin to bounce. Here is the feature of Nature that both Kelvin and Clausius disentangled from the conservation of energy: although the total quantity of energy must be conserved in any process…, the distribution of that energy changes in an irreversible manner…
I particularly like Atkins’ analysis of the equivalence of two statements of the second law: No process is possible in which the sole result is the absorption of heat from a reservoir and its complete conversion into work (Kelvin statement); and no process is possible in which the sole result is the transfer of energy from a cooler to a hotter body (Clausius statement). Atkins writes
The Clausius statement, like the Kelvin statement, identifies a fundamental dissymmetry in Nature, but ostensibly a different dissymmetry. In the Kelvin statement the dissymmetry is that between work and heat; in the Clausius statement there is no overt mention of work. The Clausius statement implies a dissymmetry in the direction of natural change: energy may flow spontaneously down the slope of temperature, not up. The twin dissymmetries are the anvils on which we shall forge the description of all natural change.
Peter Atkins has written several books, including another of my favorites: Peter Atkins’ Molecules. Here is a video of Atkins discussing his book the Four Laws that Drive the Universe. Not surprisingly, the four laws are the laws of thermodynamics.

Peter Atkins discussing the Four Laws that Drive the Universe.

Friday, November 18, 2011

Plessey Semiconductor Electric Potential Integrated Circuit

The electrocardiogram, or ECG, is one of the most common and useful tools for diagnosing heart arrhythmias. Russ Hobbie and I discuss the ECG in Chapter 7 (The Exterior Potential and the Electrocardiogram) of the 4th edition of Intermediate Physics for Medicine and Biology. The November issue of the magazine IEEE Spectrum contains an article by Willie D. Jones about new instrumentation for measuring the ECG. Jones writes
In October, Plessey Semiconductors of Roborough, England, began shipping samples of its Electric Potential Integrated Circuit (EPIC), which measures minute changes in electric fields. In videos demonstrating the technology, two sensors placed on a person’s chest delivered electrocardiogram (ECG) readings. No big deal, you say? The sensors were placed on top of the subject’s sweater, and in future iterations, the sensors could be integrated into clothes or hospital gurneys so that vital signs could be monitored continuously—without cords, awkward leads, hair-pulling sticky tape, or even the need to remove the patient’s clothes.
Apparently the Plessey device is an ultra high input impedance voltmeter. The electrode is capacitively coupled to the body, so no electrical contact is necessary. You can learn more about it by watching this video. I don’t want to sound like an advertisement for Plessey Semiconductors, but I think this device is neat. (I have no relationship with Plessey, and I have no knowledge of the quality of their product, other than what I saw in the IEEE Spectrum article and the video that Plessey produced.)

According to the Plessey press release, “most places on earth have a vertical electric field of about 100 Volts per metre. The human body is mostly water and this interacts with the electric field. EPIC technology is so sensitive that it can detect these changes at a distance and even through a solid wall.”

I don’t have any inside information about this device, but let me guess how it can detect a person at a distance. The body would perturb a surrounding electric field because it is mostly saltwater, and therefore a conductor. In Section 9.10 of Intermediate Physics for Medicine and Biology, Russ and I explain how a conductor interacts with applied electric fields. For the case of a dc field, the conducting tissue completely shields the interior of the body from the field. To understand how a body could affect an electric field, try solving the following new homework problem
Section 9.10

Problem 34 ½ Consider how a spherical conductor, of radius a, perturbs an otherwise uniform electric field, Eo. The conductor is at a uniform potential, which we take as zero. As in Problem 34, assume that the electric potential V outside the conductor is V = A cosθ/r2Eo r cosθ.
(a) Use the boundary condition that the potential is continuous at r=a to determine the constant A.
(b) In the direction θ=0, determine the upward component of the electric field, - dV/dr.
(c) The perturbation of the electric field by the conductor is the difference between the fields with and without the conductor present. Calculate this difference. How does it depend on r?
(d) Suppose you measure the voltage in two locations separated by 10 cm, and that your detector can reliably detect voltage differences of 1 mV. How far from the center of a 1 m radius conductor can you be (assuming θ=0) and still detect the perturbation caused by the conductor?
You may be wondering why there is a 100 V/m electric field at the earth’s surface. The Feynman Lectures (Volume 2, Chapter 9) has a nice discussion about electricity in the atmosphere. The reason that this electric field exists is complicated, and has to do with 1) charging of the earth by lightning, and 2) charge separation in falling raindrops.

Friday, November 11, 2011

The Making of the Pacemaker: Celebrating a Lifesaving Invention

The Making of the Pacemaker: Celebrating a Lifesaving Invention, by Wilson Greatbatch.
The Making of the Pacemaker:
Celebrating a Lifesaving Invention,
by Wilson Greatbatch.
I’m still thinking about Wilson Greatbatch, one of the inventors of the implantable pacemaker, who died a few weeks ago (see my September 30 blog entry honoring him). Here is an interesting excerpt from his book The Making of the Pacemaker: Celebrating a Lifesaving Invention, about how he created the circuit in the first pacemaker.
My marker oscillator used a 10k basebias resistor. I reached into my resistor box for one but misread the colors and got a brown-black-green (one megohm) instead of a brown-black-orange. The circuit started to ‘squeg’ with a 1.8 ms pulse, followed by a one second quiescent interval. During the interval, the transistor was cut off and drew practically no current. I stared at the thing in disbelief and then realized that this was exactly what was needed to drive a heart. I built a few more. For the next five years, most of the world’s pacemakers used a blocking oscillator with a UTC DOT-1 transformer, just because I grabbed the wrong resistor.
Here is another story from The Making of the Pacemaker about how Greatbatch met William Chardack, his primary collaborator in developing the first pacemaker.
In Buffalo we had the first local chapter in the world of the Institute of Radio Engineers, Professional Group in Medical Electronics (the IRE/PBME, now the Biomedical Engineering Society of the Institute of Electrical and Electronic Engineers [IEEE]). Every month twenty-five to seventy-five doctors and engineers met for a technical program. We strove to attract equal numbers of doctors and engineers. We had a standing offer to send an engineering team to assist any doctor who had an instrumentation problem. I went with one team to visit Dr. Chardack on a problem deadline with a blood oximeter. Imagine my surprise to find that his assistant was my old high school classmate, Dr. Andrew Gage. We couldn’t help Dr. Chardack much with his oximeter problem, but when I broached my pacemaker idea to him, he walked up and down the lab a couple times, looked at me strangely, and said, “If you can do that, you can save ten thousand lives a year.” Three weeks later we had our first model implanted in a dog.
This excerpt is interesting:
I had $2,000 in cash and enough set aside to feed my family for two years. I put it to the Lord in prayer and felt led to quit all my jobs and devote my time to the pacemaker. I gave the family money to my wife. I then took the $2,000 and went up into my wood-heated barn workshop. In two years I built fifty pacemakers, forty of which went into animals and ten into patients. We had no grant funding and asked for none. The program was successful. We got fifty pacemakers for $2,000. Today, you can’t buy one for that.
This one may be my favorite. You gotta love Eleanor. They were married in 1945 and stayed together until her death in January of this year.
Many of the early Medtronic programs were first worked out in Clarence, New York, and then taken to Minneapolis. I had two ovens set up in my bedroom. My wife did much of the testing. The shock test consisted of striking the transistor with a wooden pencil while measuring beta (current gain). We found that a metal pencil could wreck the transistor, but a wooden pencil could not. Many mornings I would awake to the cadence of my wife Eleanor tap, tap, tapping the transistors with her calibrated pencil. For some months every transistor that was used worldwide in Medtronic pacemakers got tapped in my bedroom.
You can learn more about pacemakers and defibrillators in the 4th edition of Intermediate Physics for Medicine and Biology.

A picture of Wilson Greatbatch, superimposed on Intermediate Physics for Medicine and Biology.
Wilson Greatbatch.

Friday, November 4, 2011

Countercurrent Heat Exchange

Problem 17 in Chapter 5 of the 4th edition of Intermediate Physics for Medicine and Biology considers a countercurrent heat exchanger. Countercurrent transport in general is discussed in Section 5.8 in terms of the movement of particles. However, Russ Hobbie and I conclude the section by applying the concept to heat exchange.
The principle [of countercurrent exchange] is also used to conserve heat in the extremities—such as a person’s arms and legs, whale flippers, or the leg of a duck. If a vein returning from an extremity runs closely parallel to the artery feeding the extremity, the blood in the artery will be cooled and the blood in the vein warmed. As a result, the temperature of the extremity will be lower and the heat loss to the surroundings will be reduced.
How Animals Work,  by Knut Schmidt-Nielsen, superimposed on Intermediate Physics for Medicine and Biology.
How Animals Work,
by Knut Schmidt-Nielsen.
Problem 17 provides an example of this behavior, and cites Knut Schmidt-Nielsen’s book How Animals Work (1972, Cambridge University Press), which describes countercurrent exchange in more detail. (His comments below about the nose refer to an earlier section of the book, in which Schmidt-Nielsen discusses heat exchange in the nose of the kangaroo rat).
The heat exchange in the nose has a great similarity to the well-known countercurrent heat exchange which takes place, for example, in the extremities of many aquatic animals, such as in the flippers of whales and the legs of wading birds. The body of a whale that swims in water near the freezing point is well insulated with blubber, but the thin streamlined flukes and flippers are uninsulated and highly vascularized and would have an excessive heat loss if it were not for the exchange of heat between arterial and venous blood in these structures. As the cold venous blood returns to the body from the flipper, the vessels run in close proximity to the arteries, in fact, they completely surround the artery, and heat from the arterial blood flows into the returning venous blood, which is thus reheated before it returns to the body (figure 3). Similarly, in the limbs of many animals both arteries and veins split up into a large number of parallel, intermingled vessels each with a diameter of about 1 mm or so, forming a discrete vascular bundle known as a rete…Whether the blood vessels form such a rete system, or in some other way run in close proximity, as in the flipper of the whale, is a question of design and does not alter the principle of the heat recovery mechanism. The blood flows in opposite directions in the arteries and veins, and heat exchange takes place between the two parallel sets of tubes; the system is therefore known as a countercurrent heat exchanger.
The Camel's Nose: Memoirs of a Curious Scientist, by Knut Schmidt-Nielsen, with Intermediate Physics for Medicine and Biology.
The Camel's Nose:
Memoirs of a Curious Scientist,
by Knut Schmidt-Nielsen.
Schmidt-Nielsen also wrote Scaling: Why is Animal Size So Important?, which Russ and I cite often in Chapter 2 and which I included in my top ten list of biological physics books. I have also read Schmidt-Nielsen's autobiography The Camel’s Nose: Memoirs of a Curious Scientist. (See the review of this book in the New England Journal of Medicine.) His Preface begins
This is a personal story of a life spent in science. It tells about curiosity, about finding out and finding answers. The questions I have tried to answer have been very straightforward, perhaps even simple. Do marine birds drink sea water? How do camels in hot deserts manage for days without drinking when humans could not survive without water for more than a day? How can kangaroo rats live in the desert without any water to drink? How can snails find water and food in the most barren deserts? Can crab-eating frogs really survive in sea water?

These are important questions. The answers not only tell us how animals overcome seemingly insurmountable obstacles in hostile environments; they also give us insight into general principles of life and survival.
A statue of Knut Schmidt-Nielsen with a camel on the campus of Duke University.
A statue of Knut Schmidt-Nielsen with a camel
on the campus of Duke University.
Schmidt-Nielsen died in 2007, and Steven Vogel (who I quoted in last week’s blog entry) wrote an article about him for the Biographical Memoirs of Fellows of the Royal Society (Volume 54, Pages 319–331, 2008). See also his obituary in the Journal of Experimental Biology. A statue of Schmidt-Nielsen with a camel (which he famously studied) graces the Duke University campus.