Pathogenesis/mechanism of action

Normally dietary nitrate is converted to nitrite within the reticulorumen and is slowly metabolized to ammonia. However, when present in levels that overwhelm the microbial organisms’ ability to reduce them, nitrate and nitrite are rapidly absorbed into the circulation. Once in the circulation nitrite ions readily interact with hemoglobin molecules of blood, promoting the oxidation of hemoglobin iron from the ferrous (Fe²⁺) to the ferric (Fe³⁺) state and forming methemoglobin. The methemoglobin molecule is incapable of binding and transporting oxygen molecules. Once sufficient hemoglobin is oxidized to methemoglobin, clinical signs of hypoxia develop including exercise intolerance, dyspnea, muscle tremors, and cyanotic and occasionally brown-colored membranes and blood. Although maternal methemoglobin molecules are incapable of crossing the placenta, nitrite and nitrate readily cross and can induce fetal erythrocyte methemoglobinemia and anoxia. Typically, reproductive repercussions including abortions, stillbirths, and the birth of weak calves have been reported approximately 3–7 days or more following maternal toxic exposure. In addition to the effects of methemoglobinemia, nitrite and nitrates also act as potent vasoactive compounds resulting in vasodilation and hypotension.^2,8

Diagnosis of nitrate/nitrite poisoning

In adult cattle nitrate/nitrite poisoning may be suspected based on clinical signs including brownish discoloration of the blood and mucous membranes and a history of exposure to possible nitrate-accumulating forages.^2,4 However, the characteristic chocolate-colored mucous membranes and blood are not always present and can become less obvious as autolysis proceeds.⁹

In cases of suspect nitrate toxicosis-induced abortion, a full necropsy should be performed on the fetus to rule out other potential causes. Ocular fluid from the fetus or cow can be collected for postmortem nitrate/nitrite analysis by ion chromatography with a conductivity detector. This test can be quite reliable when fluid is collected within hours of death and refrigerated. Standard nitrate dipsticks are also available and can be used to make a presumptive diagnosis of nitrate poisoning. Ideally, nitrate levels should approach 30 ppm or greater to be highly suggestive of nitrate/nitrite-associated abortion. However, a compatible history including maternal grazing on potential nitrate-accumulating forages, or some other form of excessive maternal ingestion of nitrates, is also needed.⁶ Forage nitrate analysis should also be conducted for confirmation. Forages containing greater than 0.6–1.0% nitrates (6000–10 000 ppm on a dry-matter basis) have been associated with reproductive losses (abortion, stillbirths, and weak calves).²

Treatment and management

Treatment of individual animals with intravenous methylene blue in a 1% or 2% aqueous solution at a rate of 1–2 mg/kg body weight with up to 10 mg/kg in severe cases can be performed. However, due to withdrawal times, cattle should not be sold for slaughter for up to 180 days.⁹ Although methylene blue treatment can be effective in individual animals, it is likely cost prohibitive in herd outbreaks. When nitrate/nitrite poisoning is suspected cattle should be removed from pasture. Propionibacterium acidipropionici strain P5 (a bacterial feed additive) may be supplemented if exposure to high nitrate concentrations in feed or water is unavoidable. Water should be tested when nitrate contamination is suspected from manure or fertilizer runoff. Water nitrate concentrations should be below 440 mg/L, although acute toxicity is typically not appreciated until water nitrate levels exceed 1300 mg/L.⁶

Management and treatment

There are no methods to completely prevent pine needle-induced abortions, although the potential impacts may be minimized. Ideally, pregnant cows should be denied access to pine needles when they are most susceptible to the abortifacient effects of isocupressic acid (third trimester). Pregnant cows should be maintained in adequate body condition when grazing ranges with ponderosa pines to reduce consumption. Adequate food and shelter should also be provided for cattle to minimize stress and consumption of pine needles. Calving schedules may also be changed to late spring or fall when winter weather conditions are less likely to increase pine needle ingestion.¹⁰

There is no effective treatment for pine needle toxicosis. Supportive care including antibiotic treatment and uterine infusion in cases of placental retention are recommended for cows that abort. Supplemental colostrum and milk may be required for live premature calves.¹¹

Abortions similar to those caused by ponderosa pine in cattle have also been associated with accidental ingestion of Monterey cypress (Cupressus macrocarpa) in New Zealand. Monterey cypress is a native of California that has been widely planted throughout Europe and New Zealand. Analysis of Cupressus macrocarpa in New Zealand detected elevated concentrations of isocupressic acid. Isocupressic acid is also the primary diterpene acid in Pinus contorta (lodgepole pine), Juniperus communis (common juniper), Korean pine (Pinus koraiensis), and California juniper (Juniperus californica), all of which have been associated with late-term abortions in cattle. Cattle abortions have also been attributed to the ingestion of bark from the Utah juniper (Juniperus osteosperma) and western juniper (Juniperus occidentalis), both of which contain increased concentrations of agathic acid but minimal isocupressic acid.¹³

Astragalus and Oxytropis (locoweeds)

Locoweeds, or milk vetches (Figure 65.3), include several species of plants in the genera Astragalus and Oxytropis.²³ Astragalus and Oxytropis are members of the Fabaceae (Leguminosae) or pea family. These plants are characterized by their butterfly-like flowers displaying a single large banner petal, two side petals, and two lower fused petals forming a keel. Astragalus and Oxytropis species have a worldwide distribution. Collectively, locoweeds are considered to be the most detrimental poisonous plant of cattle in the western United States and are responsible for significant economic losses.^4,30

Clinical signs of locoweed poisoning are caused by the toxic effects of the indolizidine alkaloid swainsonine found in multiple species of Astragalus and Oxytropis. Swainsonine is produced by the fungal endophyte Undifilum oxytropis (formerly Embellisia oxytropis) which can be found in the parenchymal layers of the infected plant seeds.¹¹ Locoweed poisoning is the chronic condition that develops in ruminants after weeks of ingesting swainsonine-containing plants. Common clinical signs of locoism include depression, incoordination, tremors, weight loss, emaciation, ataxia (staggering), altered mentation, belligerence, aggression, proprioceptive deficits, and eventually death. Reproductive failure, embryo loss, abortion, and occasional birth defects can be associated with locoweed poisoning and are often seen prior to more severe clinical signs in the cow.³¹

Lupines

Lupines (Lupinus spp.), commonly known as blue bonnet, belong to the Fabaceae (legume) family (Figure 65.4). These perennial herbaceous plants are indigenous to North America and range throughout much of the United States. Over 100 species of lupines have been identified. Plants grow up to 1 m high. Leaves are alternate and palmately divided with 5–17 leaflets, which can be smooth or hairy depending on the species. Flowers of Lupinus spp. are bonnet-shaped and are present on racemes that are located on a single central stalk. Poisonous varieties of lupine responsible for cattle toxicosis in the United States are predominantly found in the Rocky Mountain region and in states located to the west of the Rockies. Lupines are typically not very palatable to cattle and are most often grazed only when other forages are not readily available.^4,11

Three specific syndromes in livestock have been attributed to lupine toxicosis in North America: (i) “crooked calf disease,” a teratogenic condition caused by pregnant cows grazing lupines; (ii) acute fatal neurologic disease in adult cattle; and (iii) lupinosis. Lupinosis is not an alkaloid-induced toxicity but is instead caused by cattle grazing lupines infected with the fungus Phomopsis leptostromiformis that produces the mycotoxin phomopsin. Clinical signs of phomopsin poisoning may include severe hepatic, renal, and muscle disease in cattle and sheep.⁴ Clinical signs of the neurologic syndrome in adult cattle include muscle weakness, agitation, frequent urination and defecation, depression, frothing at the mouth, relaxation of the third eyelid, muscle fasciculations, ataxia, lethargy, collapse, and sternal recumbency followed by lateral recumbency, respiratory failure, and death.¹¹

Maternal ingestion of toxic lupines during days 40–70 of gestation results in significant fetal malformations depending on the concentration of teratogenic compounds present in the plant.²⁹ Alkaloids responsible for fetal teratogenic effects (crooked calf syndrome) include anagyrine, ammodendrine, and N-methyl-ammodendrine.¹¹

The most commonly observed lupine-induced fetal malformation is arthrogryposis of the forelimbs (Figure 65.5), which may be accompanied by scoliosis, torticollis, lordosis, kyphosis, or palatoschisis (cleft palate).^11,34 Muscles from affected limbs are often hypoplastic or atrophied. Muscle atrophy is attributed to disuse of the affected limb(s) in utero.³⁴ The mechanism of action for teratogenic fetal effects is an alkaloid-induced decrease in fetal movement secondary to desensitization of skeletal muscle-type nicotinic acetylcholine receptors. Decreased or inhibited fetal movement results in skeletal malformations including skeletal muscle contractions and cleft palate formation.¹¹

Poison hemlock (Conium maculatum)

Poison hemlock, also known as European hemlock, spotted hemlock, and California fern, is a biennial perennial member of the parsley/carrot (Apiaceae, formerly Umbelliferae) family found all across North America (Figure 65.6). Conium maculatum is one of the most toxic members of the plant kingdom.³⁵ It was originally introduced to North America from Europe as an ornamental plant and is also native to Asia but can be found throughout North and South America, North Africa, Australia, and New Zealand. Poison hemlock is a tall branched plant with distinctive purple spots along its stems, multiple small white five-petaled flowers, a single taproot, and a distinctive mousy odor.^4,31,36

Poison hemlock contains eight known piperidine alkaloids.³⁶ The two major toxic alkaloids are γ-coniceine found in immature growing plants and coniine found in mature plants and seeds.^4,31,36 However, all vegetative organs, flowers, and fruits contain alkaloids.³⁵ Alkaloid levels vary based on environmental factors (such as temperature and moisture), stage of growth, and geographic location. Fresh drying the plant in the sun for 7 days results in significantly decreased levels of the toxic piperidine alkaloids.³¹

Poison hemlock is highly toxic to cattle and in acute poisoning cases clinical signs may develop rapidly following ingestion (30 min to 1 hour). Reported clinical manifestations include depression, abdominal pain, mydriasis (dilated pupils), frequent urination and defecation, increased salivation (ptyalism), lacrimation, muscle tremors and fasciculations, incoordination and ataxia, respiratory distress, recumbency, collapse, and death. Animals surviving acute poisoning usually recover but abortions may result. The teratogenic effects of C. maculatum are most often appreciated in cases of chronic ingestion by pregnant cattle. However, fetal malformations have also been described in piglets and lambs.³⁶ Ingestion of the plant between days 40 and 70 of gestation can result in a wide array of skeletal malformations in the neonate.⁴ Reported teratogenic malformations are indistinguishable from those caused by lupines and tobacco species. Fetal malformations may include torticollis (twisted neck), scoliosis (vertebral column curvature), palatoschisis (cleft palate), arthrogryposis (multiple joint contractures), and excessive flexure of the carpal joints (crooked calf disease).^35,36

Tobacco poisoning

Nicotiana glauca (tree tobacco), Nicotiana tabacum (cultivated tobacco), Nicotiana trigonophylla (wild or desert tobacco), and Nicotiana attenuata (wild or coyote tobacco) are members of the nightshade (Solanaceae) family. Wild tobacco varieties are indigenous to the southwestern United States while cultivated tobacco grown in the United States is predominantly raised in the southeastern states. Tobacco is a herbaceous branching annual that grows between 0.3 and 1.2 m in height, with hairy stems and leaves and fragrant tubular flowers with five parts. Tree tobacco (N. glauca) is an evergreen shrub or small tree growing 2–6 m tall with alternate bluish-green hairless leaves. Flowers are 5 cm long, tubular, and produced on the leafless branches.⁴

Tobacco contains numerous alkaloids (over 40) most of which are neurotoxic pyridine alkaloids including nicotine. Animals may become intoxicated by grazing the plant or ingesting cut stalks.³⁸ In adult cattle clinical signs of acute toxicity may include excitation, followed by depression, respiratory failure, and death in severe cases. Treatment of affected animals is symptomatic. The principal toxins responsible for tobacco toxicosis in cattle are nicotine and anabasine. Nicotiana glauca produces the piperidine alkaloid anabasine, a potent nicotinic acetylcholine receptor agonist. Anabasine is acutely toxic as well as teratogenic.³⁸ Ruminants are relatively more tolerant of the neurotoxic alkaloid effects of nicotine. However, the teratogenic anabasine can induce fetal skeletal malformations including arthrogryposis, palatoschisis, torticollis, lordosis, and kyphosis. Fetal defects resulting from tobacco intoxication occur when cattle ingest the plant between days 30 and 60 of gestation.

The fetal malformations caused by tobacco toxicosis are indistinguishable from those induced by poison hemlock, locoweeds, and lupine poisoning. This similarity of teratogenic fetal malformations is attributed to the analogous molecular structures of anabasine and coniine (principal toxin of C. maculatum and lupines) and its analogs.⁴

At low doses anabasine stimulates depolarization of postsynaptic membranes of ganglia and at high does causes neuromuscular blockade. Like poison hemlock and lupine toxicosis, the mechanism of teratogenicity is believed to be caused by the neuromuscular blockade of nerves and subsequent decrease in intrauterine fetal movement resulting in the development of joint contractures, palatoschisis formation, and other skeletal malformations.^39,40 In acute toxicosis, cattle should be removed from contaminated fields or pastures. In severe cases supportive and symptomatic treatment is recommended for affected animals and may include gastric lavage.²⁸

Veratrum californicum (false hellebore)

Veratrum californicum grows in dense sharply defined stands in high moist meadows or hills.²⁹ Individual plants grow approximately 2–3 m tall and have short rootstalks and alternate smooth, broad, parallel-veined oval leaves that are present in three ranks. Numerous toxic alkaloids have been identified in V. californicum; however, the jervine alkaloids including cyclopamine, jervine, and cycloposine are associated with the plant’s teratgenic effects.^4,39 Among the toxic alkaloids, cyclopamine is present at the highest levels and is the principal teratogenic alkaloid.²⁹

Teratogenic effects are predominantly seen in sheep but fetal malformations have also been reported in goats and cattle.³³ The teratogenic alkaloids exert their effects by interfering with the sonic hedgehog (SHH) signal transduction pathway, by inhibition of neuroepithelial cell mitosis and migration, and by decreasing chondrocyte proliferation. In pregnant ewes, ingestion of V. californicum on days 12–14 of gestation (most notably day 14) results in cyclopia and prolonged gestation. Embryo death can result from maternal exposure on days 19–21. Cleft palate results from maternal exposure on gestational days 24–30 and metacarpal and metatarsal defects occur when ewes are exposed on days 28–31 of gestation.³⁹

Ingestion of V. californicum in pregnant cows between days 12 and 30 of gestation may cause fetal malformations, including cleft palate, harelip, brachygnathia, hypermobility of the hocks, syndactyly, and decreased numbers of coccygeal vertebrae. When pregnant cows ingest the plant in later stages of pregnancy (days 30–36), teratogenic alkaloids inhibit growth in length of metacarpal and metatarsal bones.³³

There is no specific treatment for V. californicum-induced fetal malformations. However, malformations can be prevented by removing pregnant animals from V. californicum-infested pastures and ranges during the first trimester of pregnancy.⁴

Mimosa spp.

Mimosa tenuiflora and Mimosa ophthalmocentra are perennial trees or small shrubs native to Brazil. Mimosa tenuiflora and possibly M. ophthalmocentra (Fabaceae, Mimosoideae) can induce fetal malformations and embryonic death in goats, sheep, and less frequently cattle. Affected calves, lambs, and kids may be born with an array of malformations, which can include arthrogryposis, micrognathia, cheiloschisis (harelip), palatoschisis, kyphosis, lordosis, torticollis, blindness, microphthalmia, corneal opacity, ocular dermoids, acephaly, bicephaly, hydranencephaly, glossal hypoplasia, meningocele, and syringocele. The toxic principle of M. tenuiflora is unknown, but tryptamine-derived alkaloids have been isolated from the leaves and seeds.¹⁷

Ergot alkaloids

Ergot alkaloids include more than 80 indole compounds and are associated with two mycotoxicoses in livestock species: fescue toxicosis and ergotism.² Both conditions may share similar clinical manifestations and in many cases may be indistinguishable from one another.⁴³ Ergot alkaloids are produced by the mold Claviceps purpurea on wheat, rye, and other cereal grains and by the endophyte Neotyphodium coenophialum growing on tall fescue (Lolium arundinaceum [Shreb]). Ergot alkaloids have similar molecular structures to the biogenic amines norepinephrine, serotonin, and dopamine and act as agonists at various serotonin receptors.^44,45 This agonistic effect is thought to be responsible for clinical manifestations of ergot alkaloid toxicosis. In both fescue toxicosis and ergotism the principal ergot alkaloid believed to be most responsible for clinical disease is ergovaline. Ergovaline is a potent α₂-adrenergic agonist on arterioles and other blood vessels causing vasoconstriction.⁴²

Tall fescue

Fescue toxicosis is one of the most costly grass-related intoxications of livestock in the United States and throughout many other countries. Fescue toxicosis is a descriptive term used for several clinical syndromes (summer slump, fescue foot, and fat necrosis) attributed to ingestion of endophyte-infected tall fescue.⁴²

Tall fescue (L. arundinaceum [Shreb]) is a cool-season perennial grass grown in temperate climates and is one of the most abundant forage crops in the continental United States.⁴⁶ In cases of fescue toxicosis, livestock ingest the fungal endophyte Neotyphodium coenophialum (formerly Acremonium coenophialum and Epichloe typhina) that grows within the intercellular spaces of the leaf sheaths, stems, and seeds of tall fescue grass.² Tall fescue and its endophyte N. coenophialum share a mutually beneficial relationship. The endophyte produces toxins (ergot alkaloids, loline alkaloids, and peramine) that are distributed throughout the plant making it more resistant to drought, parasitism, and fungal infection.⁴² The endophyte of tall fescue produces an array of ergot alkaloids but ergovaline is the primary ergopeptine alkaloid believed to be responsible for inducing toxicosis. Ergot alkaloids are highly concentrated within the seeds of tall fescue and levels are greatest in the summer and early fall when seed heads are present.⁴⁶ Drought and rainy conditions as well as fertilization with nitrogen- and phosphorus-based fertilizers tend to increase ergovaline concentrations.⁴²

Several syndromes including summer slump, fescue foot (Figure 65.7), and fat necrosis (lipomatosis) are associated with fescue toxicosis in cattle. The most costly of the three is summer slump. As the name implies clinical manifestations of this condition are most often appreciated in summer months when the ambient temperature is above 31 °C.⁴² Affected cattle typically have a rough hair coat, unthrifty appearance, reduced feed intake, decreased milk production with lower weaning weights of calves, reduced conception rates, agitation/nervousness, ptyalism, and increased respiratory rates.^42,47

Ergotism

Ergot is a general term referring to a group of parasitic fungi belonging to the genus Claviceps, most notably Claviceps purpurea, that infect rye, barley, wheat, oats, and other cereal grains.⁴⁴ Infection of grains with C. purpurea results in colonization of the grain ovary wall or base with fungal mycelia. The mycelia produce a sticky exudate called honeydew containing conidia (asexually produced spores). Following germination within the hardened honeydew (sclerotia), conidia can be transferred to and infect other seeds by insect vectors or direct contact.^44,45 Signs of ergotism – the various toxic effect(s) of ergot alkaloids produced by Claviceps spp. – develop secondary to the ingestion of toxic levels of ergot-infected grains.⁴⁴

Clinical signs of ergotism are primarily caused by the ergopeptine class of ergot alkaloids, which include ergotamine, ergocristine, ergosine, ergocornine, ergocryptine, and ergovaline. Ergot alkaloids act as serotonin receptor agonists due to the similarities of their molecular structures with the biogenic amines dopamine, serotonin, and histamine.^44,45 Vasoconstriction results from the agonistic activity of ergot alkaloids. Other potential effects include uterine stimulation and dopaminergic activity at D₂ receptors resulting in decreased prolactin secretion.⁴⁵ Documented cases of ergotism in the United States are uncommon because milling and cleaning processes are successful in removing ergot-infected grains.⁴¹

Ergot alkaloid toxicity is known to cause four distinct disease forms in livestock: (i) cutaneous and gangrenous lesions on the tail and extremities, (ii) hyperthermia and production loss, (iii) reproductive failure, and (iv) the less common and frequently debated neurologic form.^2,45 The gangrenous form of ergot poisoning represents the chronic form of intoxication by ergot-producing fungi. Clinical signs of gangrenous ergotism include acute lameness with swelling and hyperemia. Lesions present most often in the rear limbs, although all four limbs may be affected in some cases; however, necrosis is usually restricted to below the fetlock but occasionally extend to the metatarsals.²⁰ Vasoconstriction of small arteries and arterioles due to the potent α₂-adrenergic agonistic effects of ergovaline causes ischemia and necrosis of the distal limbs, ear tips, and the distal third of the tail. This gangrenous form is most often associated with winter months due to exacerbation of the vasoconstrictive effects by cold weather.⁴⁵ The hyperthermic form of the disease is the most commonly reported form of ergotism and is seen most often in summer months when weather is warm.⁴⁴ The neurologic form of ergotism appears to be rare and may be associated with acute intoxication with large doses of ergot alkaloids.⁴⁵

Aflatoxins

Aflatoxins (B₁, B₂, G₁, and G₂, named for their respective blue or green fluorescence under ultraviolet light) are a group of structurally related difuranocoumarin compounds produced primarily by Aspergillus flavus and Apergillus parasiticus. Aflatoxins can be found throughout the world and can commonly contaminate animal feed and crops in warm subtropical and tropical climates under appropriate conditions.^40,41,43 Grains stored under high moisture (>14%), at warm temperatures (>20 °C), or those improperly dried are at risk of becoming contaminated.⁵⁰ Aspergillus flavus strains invade damaged plant tissue and predominantly produce aflatoxin B₁ which is considered to be the most toxic and carcinogenic aflatoxin.⁴³

All animals are susceptible to the toxic effects of aflatoxins, although differences in species sensitivities do exist. Susceptibility can vary with breed, age, dose, nutritional status, and length of exposure.⁵⁰ Cattle and other ruminants are considered to be relatively resistant in comparison with monogastric species. However, young calves are at greater risk of developing clinical toxicosis compared with adult animals.⁴³

Aflatoxins are primarily hepatotoxic but can also have immunosuppressive, carcinogenic, mutagenic, and teratogenic effects.⁴³ Some aflatoxins have been shown to cross the placenta in laboratory animals and humans. Decreased male fertility via decreased spermatozoa production, embryo loss, fetal death, and possible teratogenic effects have been reported with aflatoxicosis, most notably with aflatoxin B₁ and G₁ in animals.⁵¹ Abortions in cattle are uncommonly reported with aflatoxicosis, but sporadic herd outbreaks have been attributed to ingestion of feeds contaminated with aflatoxin B₁, B₂, G₁, and G₂.⁴³ However, the negative reproductive impacts do not appear to be due to any direct activity of aflatoxins in the oocyte or embryo but instead are attributed to altered maternal homeostasis.⁴¹

Zearalenone

Zearalenone is a potent estrogenic mycotoxin produced by the fungus Fusarium graminearum and multiple other species of Fusarium. Zearalenone contaminates cereal grains including corn and to a lesser extent wheat, barley, sorghum, millet, rice, and oats under specific environmental and storage conditions.³⁹ Zearalenone can have profound effects on reproductive function due to its estrogenic actions. Clinical signs attributed to zearalenone toxicity are most often reported in swine, although signs may also be observed in ruminant species as well. Clinical signs of zearalenone toxicity mimic those of estrogenic stimulation and can include decreased fertility, abnormal estrous cycles, vulvar swelling, vaginitis, reduced milk production, and mammary gland enlargement. Heifers appear to be more susceptible to the effects of zearalenone than adult cows.^41,52 However, in pregnant cows the potential for abnormal embryonic or fetal development with possible fetal death, abortion, and dystocia exists.²

Zearalenone and its derivatives (α- and β-zearalenol) are believed to exert their toxic effects by competitively binding to specific estrogen receptors and by modification of steroid metabolites. Zearalenone and α- and β-zearalenol have chemical structures closely resembling naturally occurring estrogen.⁵³ Zearalenone and its metabolites can directly bind with cytoplasmic estradiol-17β receptors and translocate receptor sites to the nucleus where stimulation of RNA leads to protein synthesis and clinical signs of estrogenism.⁵² β-Zearalenol appears to be the predominant zearalenone metabolite in cattle as opposed to α-zearalenol which predominates in most other species including swine.²