Nephrolithiasis/Renal calculi/Kidney stones Formation of stones Urinary tract stone disease, depicted below, is likely caused by two basic

phenomena. The first phenomenon is supersaturation of the urine by stone-forming constituents, including calcium, oxalate, and uric acid. Crystals or foreign bodies can act as nidi, upon which ions from the supersaturated urine form microscopic crystalline structures. The resulting calculi give rise to symptoms when they become impacted within the ureter as they pass toward the urinary bladder. The overwhelming majority of renal calculi contain calcium. Uric acid calculi and crystals of uric acid, with or without other contaminating ions, comprise the bulk of the remaining minority. Other, less frequent stone types include cystine, ammonium acid urate, xanthine, dihydroxyadenine, and various rare stones related to precipitation of medications in the urinary tract. Supersaturation of the urine is likely the underlying cause of uric and cystine stones, but calcium-based stones (especially calcium oxalate stones) may have a more complex etiology. The second phenomenon, which is most likely responsible for calcium oxalate stones, is deposition of stone material on a renal papillary calcium phosphate nidus, typically a Randall plaque (which are always composed of calcium phosphate). Evan et al recently proposed this model based on evidence accumulating from several laboratories.[2] Calcium phosphate precipitates in the basement membrane of the thin loops of Henle, erodes into the interstitium, and then accumulates in the subepithelial space of the renal papilla. The subepithelial deposits, which have long been known as Randall plaques, eventually erode through the papillary urothelium. Stone matrix, calcium phosphate, and calcium oxalate gradually deposit on the substrate to create a urinary calculus. Development of renal colic pain and renal damage The colicky-type pain known as renal colic usually begins in the upper lateral midback over the costovertebral angle and occasionally subcostally. It radiates inferiorly and anteriorly toward the groin. The pain generated by renal colic is primarily caused by the dilation, stretching, and spasm caused by the acute ureteral obstruction. (When a severe but chronic obstruction develops, as in some types of cancer, it is usually painless.) In the ureter, an increase in proximal peristalsis through activation of intrinsic ureteral pacemakers may contribute to the perception of pain. Muscle spasm, increased proximal peristalsis, local inflammation, irritation, and edema at the site of obstruction may contribute to the development of pain through chemoreceptor activation and stretching of submucosal free nerve endings. The term "renal colic" is actually a misnomer, because this pain tends to remain constant, whereas intestinal or biliary colic is usually somewhat intermittent and

often comes in waves. The pattern of the pain depends on the individuals pain threshold and perception and on the speed and degree of the changes in hydrostatic pressure within the proximal ureter and renal pelvis. Ureteral peristalsis, stone migration, and tilting or twisting of the stone with subsequent intermittent obstructions may cause exacerbation or renewal of the renal colic pain. The severity of the pain depends on the degree and site of the obstruction, not on the size of the stone. A patient can often point to the site of maximum tenderness, which is likely to be the site of the ureteral obstruction (see the image below).

Nephrolithiasis: acute renal colic. Distribution of renal and ureteral pain.

A stone moving down the ureter and causing only intermittent obstruction actually may be more painful than a stone that is motionless. A constant obstruction, even if high grade, allows for various autoregulatory mechanisms and reflexes, interstitial renal edema, and pyelolymphatic and pyelovenous backflow to help diminish the renal pelvic hydrostatic pressure, which gradually helps reduce the pain. The interstitial renal edema produced stretches the renal capsule, enlarges the kidney (ie, nephromegaly), and increases renal lymphatic drainage. (Increased capillary permeability facilitates this edema.) It may also reduce the radiographic density of the affected kidneys parenchyma when viewed on a noncontrast CT scan. Distention of the renal pelvis initially stimulates ureteral hyperperistalsis, but this diminishes after 24 hours, as does renal blood flow. Peak hydrostatic renal pelvis pressure is attained within 2-5 hours after a complete obstruction. Within the first 90 minutes of a complete ureteral obstruction, afferent preglomerular arteriolar vasodilation occurs, which temporarily increases renal blood flow. Between 90 minutes and 5 hours after the obstruction, renal blood flow starts to decrease while intraureteral pressure continues to rise. By 5 hours after a complete obstruction, both renal blood flow and intraluminal ureteral pressure decrease on the affected side. Renal blood flow decreases to approximately 50% of normal baseline levels after 72 hours, to 30% after 1 week, to 20% after 2 weeks, and to 12% after 8 weeks. By this point, intraureteral pressures have returned to normal, but the proximal ureteral dilation remains and ureteral peristalsis is minimal. Interstitial edema of the affected kidney actually enhances fluid reabsorption, which helps to increase the renal lymphatic drainage to establish a new, relatively stable,

equilibrium. At the same time, renal blood flow increases in the contralateral kidney as renal function decreases in the obstructed unit. In summary, by 24 hours after a complete ureteral obstruction, the renal pelvic hydrostatic pressure has dropped because of (1) a reduction in ureteral peristalsis; (2) decreased renal arterial vascular flow, which causes a corresponding drop in urine production on the affected side; and (3) interstitial renal edema, which leads to a marked increase in renal lymphatic drainage. Additionally, as the ureter proximal to the stone distends, some urine can sometimes flow around the obstruction, relieving the proximal hydrostatic pressure and establishing a stable, relatively painless equilibrium. These factors explain why severe renal colic pain typically lasts less than 24 hours in the absence of any infection or stone movement. Whether calyceal stones cause pain continues to be controversial. In general, in the absence of infection, how a renal stone causes pain remains unclear, unless the stone also causes obstruction. Arguably, proving that a calyceal stone is causing an obstruction can be difficult. However, a stone trapped in a calyx plausibly could block the outflow tract from that calyx, causing an obstruction and subsequent pain. Experimental studies in animals have suggested that renal damage may begin within 24 hours of a complete obstruction and that permanent kidney deterioration starts within 5-14 days. Whereas some practitioners wait several months for a stone to pass in an asymptomatic patient, others argue that permanent damage is occurring as long as intervention is delayed. Based on personal experience and anecdotal cases, the author recommends waiting no longer than 4 weeks for a stone to pass spontaneously before considering intervention. Convincing asymptomatic patients of the need for surgical intervention may be difficult in the absence of a clear consensus in the urological community about the length of time to wait before surgical stone removal, fragmentation, or bypass. If only a partial obstruction is present, the same changes occur, but to a lesser degree and over a longer period. Proximal ureteric and renal pelvic hydrostatic pressures tend to remain elevated longer, and ureteral peristalsis does not diminish as quickly. If the increased pressure is sufficient to establish a reasonable flow beyond the obstructing stone, glomerular filtration and renal blood flow approximates reference range baseline levels, although pain may be ongoing.

Etiology
A low fluid intake, with a subsequent low volume of urine production, produces high concentrations of stone-forming solutes in the urine. This is an important, if not the most important, environmental factor in kidney stone formation. The exact nature of the tubular damage or dysfunction that leads to stone formation has not been characterized.

Most research on the etiology and prevention of urinary tract stone disease has been directed toward the role of elevated urinary levels of calcium, oxalate, and uric acid in stone formation, as well as reduced urinary citrate levels. Hypercalciuria is the most common metabolic abnormality. Some cases of hypercalciuria are related to increased intestinal absorption of calcium (associated with excess dietary calcium and/or overactive calcium absorption mechanisms), some are related to excess resorption of calcium from bone (ie, hyperparathyroidism), and some are related to an inability of the renal tubules to properly reclaim calcium in the glomerular filtrate (renal-leak hypercalciuria). Magnesium and especially citrate are important inhibitors of stone formation in the urinary tract. Decreased levels of these in the urine predispose to stone formation. The following are the 4 main chemical types of renal calculi, which together are associated with more than 20 underlying etiologies: Calcium stones Struvite (magnesium ammonium phosphate) stones Uric acid stones Cystine stones Stone analysis, together with serum and 24-hour urine metabolic evaluation, can identify an etiology in more than 95% of patients. Specific therapy can result in a remission rate of more than 80% and can decrease the individual recurrence rate by 90%. Therefore, emergency physicians should stress the importance of urologic follow-up, especially in patients with recurrent stones, solitary kidneys, or previous kidney or stone surgery and in all children.[3] Calcium stones Calcium stones account for 75% of renal calculi. Recent data suggest that a lowprotein, low-salt diet may be preferable to a low-calcium diet in hypercalciuric stone formers for preventing stone recurrences.[4] Epidemiological studies have shown that the incidence of stone disease is inversely related to the magnitude of dietary calcium intake in first-time stone formers. There is a trend in the urology community not to restrict dietary intake of calcium in recurrent stone formers. This is especially important for postmenopausal women in whom there is an increased concern for the development of osteoporosis. Calcium oxalate, calcium phosphate, and calcium urate are associated with the following disorders:
Hyperparathyroidism - Treated surgically or with orthophosphates if the patient

is not a surgical candidate Increased gut absorption of calcium - The most common identifiable cause of hypercalciuria, treated with calcium binders or thiazides plus potassium citrate Renal calcium leak - Treated with thiazide diuretics Renal phosphate leak - Treated with oral phosphate supplements

 Hyperuricosuria - Treated with allopurinol, low purine diet, or alkalinizing agents

such as potassium citrate Hyperoxaluria - Treated with dietary oxalate restriction, oxalate binders, vitamin B-6, or orthophosphates Hypocitraturia - Treated with potassium citrate Hypomagnesuria - Treated with magnesium supplements Struvite (magnesium ammonium phosphate) stones Struvite stones account for 15% of renal calculi. They are associated with chronic urinary tract infection (UTI) with gram-negative rods capable of splitting urea into ammonium, which combines with phosphate and magnesium. Usual organisms include Proteus, Pseudomonas, and Klebsiella species. Escherichia coli is not capable of splitting urea and, therefore, is not associated with struvite stones. Urine pH is typically greater than 7. Underlying anatomical abnormalities that predispose patients to recurrent kidney infections should be sought and corrected. UTI does not resolve until stone is removed entirely. Uric acid stones Uric acid stones account for 6% of renal calculi. These are associated with urine pH less than 5.5, high purine intake (eg, organ meats, legumes, fish, meat extracts, gravies), or malignancy (ie, rapid cell turnover). Approximately 25% of patients with uric acid stone have gout. Serum and 24-hour urine sample should be sent for creatinine and uric acid determination. If serum or urinary uric acid is elevated, the patient may be treated with allopurinol 300 mg daily. Patients with normal serum or urinary uric acid are best managed by alkali therapy alone. Cystine stones Cystine stones account for 2% of renal calculi. They arise because of an intrinsic metabolic defect resulting in failure of renal tubular reabsorption of cystine, ornithine, lysine, and arginine. Urine becomes supersaturated with cystine, with resultant crystal deposition. Cystine stones are treated with a low-methionine diet (unpleasant), binders such as penicillamine or a-mercaptopropionylglycine, large urinary volumes, or alkalinizing agents. A 24-hour quantitative urinary cystine determination helps to titrate the dose of drug therapy to achieve a urinary cystine concentration of less than 300 mg/L. Drug-induced stone disease A number of medications or their metabolites can precipitate in urine causing stone formation. These include indinavir; atazanavir; guaifenesin; triamterene; silicate (overuse of antacids containing magnesium silicate); and sulfa drugs including sulfasalazine, sulfadiazine, acetylsulfamethoxazole, acetylsulfasoxazole, and acetylsulfaguanidine.