Hypercalcemia Associated with Cancer

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Hypercalcemia Associated with Cancer

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Title: Hypercalcemia Associated with Cancer

1
Hypercalcemia Associated with Cancer

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Andrew F. Stewart, M.D.
N Engl J Med 2005 Volume 352373-379 January 27,
2005 Number 4

2
Outline

Case report
The Clinical Problem
Strategies and Evidence
Dx
Therapeutic Considerations
General Supportive Measures
Saline Hydration and Calciuresis
Medications
Other Pharmacologic Agents
Dialysis
Areas of Uncertainty
Guidelines
Recommendations

3
Case report

A 47-year-old woman with a history of breast
cancer presents with confusion and dehydration.
The serum Ca is 18.0 mg /dl (4.5 mmol /l). She
has postural hypotension and low central venous
pressure on examination of the jugular veins.
The serum phosphorus is 5.0 mg /dl (1.6 mmol
/l), the BUN is 80.0 mg /dl (28.6 mmol /l), the
serum Cr is 2.0 mg /dl (177 µmol /l), and the
Alb is 3.3 g /dl.
A bone scintigraphic scan reveals no evidence of
skeletal involvement by the tumor.
How should she be treated?

4
The Clinical Problem (1)

Hypercalcemia has been reported to occur in up to
20 to 30 of p'ts with cancer at some time
during the course of their disease.
This incidence may be falling owing to the wide
use of bisphosphonates in p'ts with either
multiple myeloma or breast cancer, although data
are lacking.
Hypercalcemia leads to progressive mental
impairment, including coma, as well as renal
failure. These complications are particularly
common terminal events among p'ts with cancer.
The detection of hypercalcemia in a p't with
cancer signifies a very poor prognosis 50 of
such p'ts die within 30 days.

5
Cancer-associated hypercalcemia morbidity and
mortality. Clinical experience in 126 treated
p'ts.

STUDY OBJECTIVE To review the effects of
antihypercalcemic Tx on morbidity and mortality
in cancer-associated hypercalcemia.
DESIGN Retrospective study of 126 consecutive
p'ts with cancer-associated hypercalcemia.
SETTING Inp't referrals from a teaching hospital
in the United Kingdom.
INTERVENTION Medical antihypercalcemic therapy
supplemented by specific anticancer therapy where
possible.

Ann Intern Med 1990112499-504
6

MEASUREMENTS AND MAIN RESULTS Median survival
was 30 days. Survival did not differ in p'ts
treated with different antihypercalcemic regimens
but was longer (median, 135 days P less than
0.001) in a subgroup of 26 p'ts for whom specific
anticancer therapy was available. Polyuria and
polydipsia improved after therapy in 83 of
cases, central nervous system symptoms in 71,
constipation in 70 , nausea and vomiting in 56,
anorexia in 50, and malaise and fatigue in 47
(all significant, P less than 0.001, pre-Tx
compared with post-Tx). Pain control improved in
only 23 of cases (not significant). Only 7 of
p'ts with post-Tx serum Ca values above 3.50
mmol/L improved clinically compared with 80
whose Ca values fell below 2.80 mmol/L (P less
than 0.001). Corresponding figures for the
proportion of p'ts discharged from the hospital
were 0 and 68 (P less than 0.001).
CONCLUSIONS Life expectancy is poor in
cancer-associated hypercalcemia even in p'ts who
are actively treated. Antihypercalcemic therapy
has an important palliative role, however,
because symptoms are usually improved and, in
many cases, p'ts may be made well enough to be
discharged from the hospital during the terminal
stages of their illness.

Ann Intern Med 1990112499-504
7
The Clinical Problem (2)

Hypercalcemia with cancer can be classified into
four types (Table 1).
In p'ts with local osteolytic hypercalcemia, the
hypercalcemia results from the marked increase in
osteoclastic bone resorption in areas surrounding
the malignant cells within the marrow space.
The condition known as humoral hypercalcemia of
malignancy (HHM) is caused by systemic secretion
of PTHrP by malignant tumors.
PTHrP causes increased bone resorption and
enhances renal retention of Ca. The tumors that
most commonly cause HHM are listed in Table 1,
but essentially any tumor may cause this
syndrome.
Some lymphomas secrete the active form of vitamin
D, 1,25(OH)2D, causing hypercalcemia as a result
of the combination of enhanced osteoclastic bone
resorption and enhanced intestinal absorption of
Ca.
Finally, ectopic secretion of authentic PTH is a
rare cause of hypercalcemia, having been well
documented in only eight p'ts to date.

8
Figure 2. Regulation of Bone Resorption (Panel A)
and Bone Formation (Panel B).

Both systemic factors and locally acting factors
induce the formation and activity of osteoclasts
(Panel A). Systemic hormones such as PTH,
1,25(OH)2D, and thyroxine (T4) stimulate the
formation of osteoclasts by inducing the
expression of receptor activator of nuclear
factor-?B ligand (RANKL) on marrow stromal cells
and osteoblasts.
In addition, osteoblasts produce IL-6, IL-1,
prostaglandins, and colony-stimulating factors
(CSFs), which induce the formation of
osteoclasts. Accessory cells such as T cells can
produce cytokines that can inhibit the formation
of osteoclasts, such as IL-4, IL-18, and
interferon-?. TGF-ßdenotes transforming growth
factorß . Plus signs indicate stimulation, and
minus signs inhibition.

Both systemic factors and locally acting factors
can enhance the proliferation and differentiation
of osteoblasts (Panel B). These include PTH,
prostaglandins, and cytokines as well as growth
factors such as platelet-derived growth factor
(PDGF) produced by lymphocytes.
In addition, bone matrix is a major source of
growth factors, which can enhance the
proliferation and differentiation of osteoblasts.
These include the bone morphogenetic proteins
(BMPs), TGF-ß, insulin-like growth factors
(IGFs), and fibroblast growth factors (FGFs).
Corticosteroids can induce apoptosis of
osteoblasts and block bone formation.

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12
Strategies and Evidence ---Dx (1)

Although clinical laboratories generally measure
the total serum Ca , it is occasionally valuable
to measure the serum ionized Ca, because
increases or decreases in the Alb may cause
misleading increases or decreases, respectively,
in the total serum Ca .
In addition, in rare p'ts with myeloma in whom
Ca-binding immunoglobulins are produced,
measurement of total serum Ca may substantially
overestimate the serum ionized Ca .
There are formulas with which to calculate the
serum ionized Ca or to "correct" the total Ca
(e.g., add 0.8 mg /dl to the total Ca for every
1.0 g /dl of serum Alb below the of 3.5 g /dl),
but they are not precise or always reliable.
Thus, measurement of serum ionized Ca should be
considered whenever there is doubt about the
validity of the measurement of total Ca. The test
can be performed rapidly in most hospital
laboratories or neonatal ICUs.

13
Strategies and Evidence ---Dx (2)

If the Ca is elevated, a further evaluation
should consider not only the mechanisms that are
potentially related to the cancer but also causes
of the elevation of the Ca that are unrelated to
the cancer (e.g., primary hyperparathyroidism,
the use of thiazide diuretics, and granulomatous
disease, among other causes).
The tumors present in hypercalcemia associated
with malignant disease are generally large and
readily apparent notable exceptions are small
neuroendocrine tumors (such as islet tumors and
pheochromocytomas).
Intact PTH should be measured routinely. Although
ectopic hyperparathyroidism is extremely rare in
hypercalcemia associated with cancer, concomitant
primary hyperparathyroidism is not (we found that
in 8 of 133 p'ts with cancer and hypercalcemia,
primary hyperparathyroidism was the cause).

14
Strategies and Evidence ---Dx (3)

Although most p'ts with typical HHM (Table 1)
have increased circulating PTHrP, the Dx is
usually obvious on clinical grounds PTHrP should
therefore be measured in the occasional cases in
which the Dx of HHM cannot be made on clinical
grounds or when the cause of hypercalcemia is
obscure.
Plasma 1,25(OH)2D should be measured when
sarcoidosis, other granulomatous disorders, or
the 1,25(OH)2D lymphoma syndrome is considered in
the differential Dx.
A bone scan (or a skeletal survey, in the case of
myeloma) is useful to assess the skeletal tumor
burden in p'ts with cancer and hypercalcemia, if
the test was not previously performed for tumor
staging.

15
Therapeutic Considerations (1)

In planning therapy for p'ts with hypercalcemia
associated with malignant disease,
antihypercalcemic therapy should be considered an
interim measure, one with no ultimate effect on
survival.
Thus, it is imperative that antitumor therapy be
implemented promptly control of the serum Ca
merely buys time in which such therapy can work.
Another critical point is that when all the
available therapies have failed, withholding
antihypercalcemic therapy (which will eventually
result in coma and death) may be an appropriate
and humane approach.
In cases in which Tx is considered appropriate,
an assessment of the severity of the
hypercalcemia is needed to guide therapy.

16
Therapeutic Considerations (2)

Although there are no formal guidelines, I
consider mild hypercalcemia to be a serum Ca of
10.5 to 11.9 mg /dl (2.6 to 2.9 mmol /l),
moderate hypercalcemia 12.0 to 13.9 mg /dl (3.0
to 3.4 mmol /l), and severe hypercalcemia 14.0
mg /dl (3.5 mmol /l) or greater.
In general, the neurologic and renal
complications of hypercalcemia worsen with
increasing severity of hypercalcemia, but other
factors also influence the response to
hypercalcemia. For example, the rate of the
ascent of the serum Ca is important a rapid
increase to moderate hypercalcemia frequently
results in marked neurologic dysfunction, whereas
chronic severe hypercalcemia may cause only
minimal neurologic symptoms.
Similarly, older p'ts with preexisting neurologic
or cognitive dysfunction may become severely
obtunded in the presence of mild hypercalcemia,
whereas younger p'ts with moderate-to-severe
hypercalcemia may remain alert.
Finally, the concomitant administration of
sedatives or narcotics may worsen the neurologic
response to hypercalcemia.

17
Therapeutic Considerations (3)

The optimal therapy for hypercalcemia associated
with cancer is one that is tailored both to the
degree of hypercalcemia and to its underlying
cause.
True hypercalcemia (i.e., an elevated serum
ionized Ca) occurs through three basic
mechanisms enhanced osteoclastic bone resorption
(in local osteolytic hypercalcemia, HHM,
1,25(OH)2D-secreting lymphomas, and the rare case
of ectopic hyperparathyroidism) enhanced renal
tubular reabsorption of Ca (in HHM and ectopic
hyperparathyroidism) and enhanced intestinal
absorption of Ca (in 1,25(OH)2D-secreting
lymphomas and possibly ectopic hyperparathyroidism
).
Therapy should be targeted accordingly.

18
General Supportive Measures (1)

The important general supportive measures include
the removal of Ca from parenteral feeding
solutions (a measure often overlooked)
discontinuation of the use of oral Ca supplements
in enteral feeding solutions or as Ca tablets
discontinuation of medications that may
independently lead to hypercalcemia (e.g.,
lithium, calcitriol, vitamin D, and thiazides)
an increase in the weight-bearing mobility of the
p't, if possible and discontinuation of the use
of sedative drugs, including analgesic drugs, if
possible, to enhance the p't's mental clarity and
promote weight-bearing ambulation.

19
General Supportive Measures (2)

Hypophosphatemia develops in most p'ts with
hypercalcemia associated with cancer at some
point during the course of the disease,
regardless of the underlying cause, because of
decreased food intake, saline diuresis, the use
of loop diuretics, the phosphaturic effects of
PTHrP, the hypercalcemia itself, and Tx with
calcitonin or antacids.
In general, the presence of hypophosphatemia
increases the difficulty of treating the
hypercalcemia, and in animal models
hypophosphatemia has been shown to cause
hypercalcemia.
Phosphorus should be replaced orally or
administered through a nasogastric tube as
neutral phosphate.

20
General Supportive Measures (3)

The serum phosphorus and Cr should be followed
closely, in an effort to keep the phosphorus in
the range of 2.5 to 3.0 mg /dl (0.98 to 1.0 mmol
/l), the serum Cr in the normal range, and the
Caphosphorus product below 40, ideally in the
range of 30 (when both are expressed in mg/dl).
IV phosphorus replacement should not be given
except in dire circumstances, when oral or NG
administration is impossible, because its use can
result in severe hypocalcemia, seizures, and
acute renal failure.
These general support measures alone may be
sufficient to treat p'ts with mild hypercalcemia.

21
Saline Hydration and Calciuresis (1)

P'ts with hypercalcemia associated with cancer
are substantially dehydrated as a result of a
renal water-concentrating defect (nephrogenic DI)
induced by hypercalcemia and by decreased oral
hydration resulting from anorexia and nausea,
vomiting, or both.
The dehydration leads to a reduction in the GFR
that further reduces the ability of the kidney to
excrete the excess serum Ca.
First, therefore, parenteral volume expansion
should be initiated, with the administration of
NS. Although there are no randomized clinical
trials to guide this therapy, in general practice
NS is administered at a rate of 200 to 500 ml
/hr, depending on the baseline of dehydration
and renal function, the p't's CV status, the
degree of mental impairment, and the severity of
the hypercalcemia.
These factors must be assessed with the use of
careful clinical monitoring for physical findings
that are consistent with fluid overload.

22
Saline Hydration and Calciuresis (2)

The goals of Tx are to increase the GFR, thus
increasing the filtered load of Ca that passes
through the glomerulus into the tubular lumen,
and to inhibit Ca reabsorption in the proximal
nephron (because saline itself is calciuretic).
Increasing the GFR to or above the normal range
(within safe limits) also permits the use of loop
diuretics (Table 2) to increase the renal
excretion of Ca (loop diuretics block Ca
reabsorption in the loop of Henle and make
possible increased administration of saline,
which induces further Ca excretion).
Loop diuretics should not be administered until
after full hydration has been achieved, because
these agents can cause or worsen dehydration,
leading to a decline in the GFR and the filtered
load of Ca.
In contrast to loop diuretics, thiazide diuretics
should not be administered, since they stimulate,
rather than inhibit, renal Ca reabsorption.

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24
Medications (1)

IV bisphosphonates are by far the best studied,
safest, and most effective agents for use in p'ts
with hypercalcemia associated with cancer. These
drugs work by blocking osteoclastic bone
resorption.
Because they are poorly absorbed when given
orally ( 1 to 2 of an oral dose is absorbed),
only IV bisphosphonates are used for this
indication. In the USA, the two drugs approved by
FDA and are currently considered the agents of
choice in the Tx of mild-to-severe hypercalcemia
associated with cancer are pamidronate and
zoledronate.
In continental Europe, the United Kingdom, and
other countries, ibandronate and clodronate are
also widely used. Etidronate, which was the first
to be used for this indication, has been replaced
by these more potent bisphosphonates.
A number of randomized clinical trials comparing
bisphosphonates to saline and diuretics alone, to
other bisphosphonates, and to other
antiresorptive agents such as calcitonin have
confirmed the superiority of bisphosphonates.

25
Medications (2)

Bisphosphonate therapy should be initiated as
soon as hypercalcemia is discovered, because a
response requires two to four days, and the nadir
in serum Ca generally occurs within four to seven
days after therapy is initiated.
60 to 90 of p'ts have normal serum Ca within
four to seven days, and responses last for one to
three weeks.
As compared with pamidronate, zoledronate has the
advantage of rapid and simpler administration (15
minutes vs. 2 hours for infusion), whereas
pamidronate is less expensive. Although a direct
comparison of the two drugs in a randomized
clinical trial showed a statistically significant
increase in the efficacy of zoledronate, the
difference in control of calcemia was small (mean
nadir serum Ca , 9.8 mg /dl 2.4 mmol /l with
zoledronate and 10.5 mg /dl 2.6 mmol /l with
pamidronate the proportion of p'ts in whom a
corrected serum Ca of 10.8 mg /dl 2.7 mmol /l
was achieved by day 10 was 88 and 70 ,
respectively).
Thus, the differences are of arguable clinical
importance, and the choice is largely one between
convenience and cost. Either pamidronate or
zoledronate is acceptable therapy.

26
Single-dose IV therapy with pamidronate for the
Tx of hypercalcemia of malignancy comparison of
30-, 60-, and 90-mg dosages

PURPOSE To determine the efficacy, dose-response
relationship, and safety of 30, 60, and 90 mg of
a single IV dose of an aminobisphosphonate,
pamidronate (APD), for the Tx of moderate to
severe hypercalcemia of malignancy.
P'ts AND METHODS P'ts with histologically proven
cancer and a corrected serum Ca of at least 12.0
mg/dL after 48 hours of NS hydration were
enrolled in a double-blind, multicenter,
randomized clinical trial. Pamidronate in 30-,
60-, or 90-mg doses was administered as a single
24-hour infusion. Serum Ca corrected for Alb,
urine hydroxyproline, and Ca excretion, and serum
PTH (1-84) were determined before and after
pamidronate therapy.

Am J Med 199395297-304
27

RESULTS Thirty-two men and 18 women entered the
study. A dose-response relationship for
normalization of corrected serum Ca was seen
after pamidronate administration. Corrected serum
Ca normalized in 40 of p'ts who received 30 mg,
in 61 of p'ts who received 60 mg, and in 100 of
p'ts who received 90 mg of pamidronate. The
decline in the serum Ca was associated with
decreased osteoclastic skeletal resorption
evidenced by a decrease in urine Ca and
hydroxyproline excretion. Among those with a
normalized corrected serum Ca , the mean (median)
duration of normalization of the corrected serum
Ca value was 9.2 (4), 13.3 (5), and 10.8 (6) days
in the 30-, 60-, and 90-mg Tx groups,
respectively. The response of hypercalcemia to
pamidronate was not significantly influenced by
the presence of skeletal metastases. PTH 1-84,
suppressed in p'ts on entry into this study,
increased to a greater extent in those p'ts with
osteolytic skeletal metastases compared with
those with humoral hypercalcemia of malignancy.
Clinical improvement, including improved mental
status and decreased anorexia, accompanied the
decline in the corrected serum Ca in all three
Tx groups. Side effects included low-grade fever,
asymptomatic hypocalcemia, hypomagnesemia, and
hypophosphatemia.
CONCLUSIONS A single-dose infusion of 60 to 90
mg of pamidronate was highly effective and well
tolerated and normalized corrected serum Ca in
nearly all p'ts (61 to 100) with hypercalcemia
of malignancy.

Am J Med 199395297-304
28
Zoledronic Acid Is Superior to Pamidronate in the
Tx of Hypercalcemia of Malignancy A Pooled
Analysis of Two Randomized, Controlled Clinical
Trials

PURPOSE Two identical, concurrent, parallel,
multicenter, randomized, double-blind,
double-dummy trials were conducted to compare the
efficacy and safety of zoledronic acid and
pamidronate for treating hypercalcemia of
malignancy (HCM).
P'ts AND METHODS P'ts with moderate to severe
HCM (corrected serum Ca CSC 3.00 mmol/L 12.0
mg/dL) were treated with a single dose of
zoledronic acid (4 or 8 mg) via 5-minute infusion
or pamidronate (90 mg) via 2-hour infusion. A
protocol-specified pooled analysis of the two
parallel trials was performed. Clinical end
points included rate of complete response by day
10, response duration, and time to relapse.

J Clin Oncol 200119558-567.
29

RESULTS Two hundred eighty-seven p'ts were
randomized and evaluated for safety 275 were
evaluated for efficacy. Both doses of zoledronic
acid were superior to pamidronate in the Tx of
HCM. The complete response rates by day 10 were
88.4 (P .002), 86.7 (P .015), and 69.7 for
zoledronic acid 4 mg and 8 mg and pamidronate 90
mg, respectively. Normalization of CSC occurred
by day 4 in 50 of p'ts treated with zoledronic
acid and in only 33.3 of the pamidronate-treated
p'ts. The median duration of complete response
favored zoledronic acid 4 and 8 mg over
pamidronate 90 mg with response durations of 32,
43, and 18 days, respectively.
CONCLUSION Zoledronic acid is superior to
pamidronate 4 mg is the dose recommended for
initial Tx of HCM and 8 mg for relapsed or
refractory hypercalcemia.

J Clin Oncol 200119558-567.
30
Medications (3)

In animal models, bisphosphonates have been
associated with azotemia and thus, their use in
p'ts with renal failure is a potential concern.
However, because hypercalcemia is a frequent
cause of renal dysfunction in p'ts with
hypercalcemia associated with cancer, effective
Tx of the hypercalcemia associated with cancer
often improves renal function.
The manufacturer and the American Society of
Clinical Oncology do not recommend the use of a
reduced dose of pamidronate or zoledronate for
p'ts with serum Cr values of less than 3.0 mg /dl
(265.2 µmol /l), but they do advise that the
recommended duration of the infusion not be
shortened.
Pamidronate and zoledronate have been reported to
cause or exacerbate renal failure, but this
effect has generally occurred in p'ts receiving
multiple doses.
In p'ts whose condition fails to respond to a low
initial dose of bisphosphonates, the use of a
second, larger dose (an approach that has not
been approved by the FDA) or a second-line agent
may be considered.

31
Zoledronic acid

Zoledronic acid (zoledronate) is a new generation
bisphosphonate that inhibits osteoclast bone
resorption.
It was much more potent than other
bisphosphonates at inhibiting 1,25(OH)2D-induced
hypercalcaemia in a rat model and Ca release in
vitro. A single 5-minute IV infusion of
zoledronic acid (4 or 8 mg) was significantly
more effective than a 2-hour infusion of
pamidronic acid (pamidronic acid disodium,
pamidronate disodium) 90 mg in normalising
serum Ca in p'ts with hypercalcaemia of
malignancy and resulted in a significantly longer
median time to relapse (pooled analysis from 2
randomised, double-blind, parallel-group trials).
There were no differences in tolerability between
zoledronic acid and pamidronic acid in
comparative trials the most common events in
pivotal trials were fever, anaemia, nausea,
constipation and dyspnoea.
Fever, hypophosphataemia and hypocalcaemia were
the most common events in a small phase I trial.

Drugs 200161799-805
32
Toxic acute tubular necrosis following Tx with
zoledronate (Zometa)

BACKGROUND Renal failure and toxic acute tubular
necrosis (ATN) may be seen following exposure to
a variety of therapeutic agents. Zoledronate
(Zometa) is a new, highly potent bisphosphonate
used in the Tx of hypercalcemia of malignancy. We
report the first clinical-pathologic study of
nephrotoxicity associated with this agent.
METHODS A cohort of six p'ts (four males and two
females) with a mean age of 69.2 years received
bisphosphonate therapy for multiple myeloma (five
p'ts) or Paget's disease (one p't). In all p'ts,
zoledronate was administered at a dose of 4 mg IV
monthly, infused over at least 15 minutes, and
the duration of therapy was mean 4.7 months
(range, 3 to 9 months).

Kidney Int 200364281-289
33

RESULTS All p'ts developed renal failure with a
rise in serum Cr from a mean baseline of 1.4
mg/dL to 3.4 mg/dL. Renal biopsy revealed toxic
ATN, characterized by tubular cell degeneration,
loss of brush border, and apoptosis.
Immunohistochemical staining revealed a marked
increase in cell cycle-engaged cells (Ki-67
positive) and derangement in tubular
Na,K-ATPase expression. Importantly, although
all p'ts had been treated with pamidronate prior
to zoledronate, no biopsy exhibited the
characteristic pattern of collapsing focal
segmental glomerulosclerosis observed in
pamidronate nephrotoxicity. Following renal
biopsy, Tx with zoledronate was discontinued and
all six p'ts had a subsequent improvement in
renal function (mean final serum Cr, 2.3 mg/dL at
1 to 4 months of follow-up).
CONCLUSION The close temporal relationship
between zoledronate administration and the onset
of renal failure and the partial recovery of
renal function following drug withdrawal strongly
implicate this important and widely used agent in
the development of toxic ATN.

Kidney Int 200364281-289
34
Other Pharmacologic Agents

Several agents commonly used before the advent of
bisphosphonates are now used infrequently,
usually when bisphosphonates are ineffective or
contraindicated (Table 2).
Glucocorticoids may still have a role in the Tx
of some p'ts, such as those with lymphomas
resulting in elevated s of 1,25(OH)2 vitamin D.
Calcitonin may result in a more rapid reduction
in serum Ca than do other agents (the maximal
response occurs within 12 to 24 hours), but its
value is questionable because the reductions are
small ( 1.0 mg /dl 0.25 mmol /l) and transient.
Mithramycin, which was the mainstay of therapy
for hypercalcemia associated with cancer before
the bisphosphonates became available, remains
effective, but its use is limited by potential
adverse effects (Table 2).
Gallium nitrate is also approved for Tx, but the
need for continuous IV administration over a
period of five days limits its use.

35
Effect of calcitonin and glucocorticoids in
combination on the hypercalcemia of malignancy.

The effects of the combination of glucocorticoids
and calcitonin on serum Ca were compared with the
responses to calcitonin alone in 14 p'ts with
malignant disease and hypercalcemia.
The serum Ca of those p'ts treated with
calcitonin alone returned to preTx levels within
48 hours, whereas those treated with the
combination of calcitonin and glucocorticoids
maintained the lower serum Ca for more than 4
days.
These results suggest that the combination of
calcitonin and glucocorticoids is a rapidly
effective form of medical Tx for hypercalcemia
and that glucocorticoids help to maintain the
acute response to calcitonin in p'ts with
hypercalcemia.

Ann Intern Med 198093269-272
36
Dialysis

In p'ts who have cancers that are likely to
respond to therapy but in whom acute or chronic
renal failure is present, aggressive saline
infusion is not possible, and other therapies
such as bisphosphonates should be used with
caution, if at all.
In these circumstances, dialysis against a
dialysate containing little or no Ca is a
reasonable and highly effective option for
selected p'ts.
There are no specific guidelines with regard to
how low the GFR must be for dialysis to be a
rational choice in treating hypercalcemia, but in
general, when the rate falls below 10 to 20 ml
/min, or when the presence of CHF contraindicates
an adequate administration of saline, or both,
dialysis should be considered.

37
Ca-free HD for the management of hypercalcemia

The drug therapies for hypercalcemia of
malignancy have been known to be associated with
either limited efficacy or cumulative toxicity in
p'ts with advanced renal failure.
To establish the guidelines for the use of
dialysis and to determine its optimal
prescription for hypercalcemia, Ca-free HD was
performed in 6 hypercalcemic p'ts with renal
failure not responding enough to forced saline
diuresis.
Ca-free dialysate contained Na 135, K 2.5, Cl
108, Mg 0.75, bicarbonate 30 mmol/l. Mean HD time
was 160 /- 27 min and mean Kt/V urea was 0.75
/- 0.2. Plasma Ca fell from a mean value of
2.92 /- 0.21 mmol/l (range 2.55-3.25) to 2.58
/- 0.16 mmol/l at 1 h of HD and to 2.16 /- 0.33
mmol/l (range 1.63-2.53) following 2-3 h of HD.
The ionized Ca (n 4) decreased from 1.44 /-
0.14 mmol/l to 0.99 /- 0.2 mmol/l. No p't showed
any hypocalcemic symptoms and signs during HD.
The rate of decrease in plasma Ca did not appear
to produce adverse effects in any of the p'ts.
There was a significant positive correlation
between the decrease in plasma Ca and the Kt/V
urea (y 1.4x - 0.29, r 0.92, p lt 0.01).
We conclude that Ca-free HD is indicated when the
presence of severe renal failure prevents the
administration of large volumes of IV fluids to
hypercalcemic p'ts. The amount of dialysis (Kt/V
urea) can be used to predict the decrease in
plasma Ca during Ca-free HD.

Nephron 199672424-428
38
Areas of Uncertainty (1)

The receptor activator of nuclear factor-?B
ligand (RANKL) system is the molecular pathway
that leads to osteoclast recruitment and
differentiation and bone resorption in
hypercalcemia associated with cancer.
Agents that interfere with the system, such as
recombinant osteoprotegerin (a decoy receptor for
RANKL) or monoclonal antibodies directed against
RANKL, have been proposed as novel Txs for
hypercalcemia associated with malignant disease,
as have monoclonal antibodies, which neutralize
PTHrP.

39
The Inhibition of RANKL Causes Greater
Suppression of Bone Resorption and Hypercalcemia
Compared with Bisphosphonates in Two Models of
HHM

HHM is mediated primarily by skeletal and renal
responses to tumor-derived PTHrP. PTHrP mobilizes
Ca from bone by inducing the expression of
receptor activator for nuclear factor- ?B ligand
(RANKL), a protein that is essential for
osteoclast formation, activation, and survival.
RANKL does not influence renal Ca reabsorption,
so RANKL inhibition is a rational approach to
selectively block, and thereby reveal, the
relative contribution of bone Ca to HHM.

Endocrinology, August 1, 2005 146(8) 3235 -
3243.
40

We used the RANKL inhibitor osteoprotegerin (OPG)
to evaluate the role of osteoclast-mediated
hypercalcemia in two murine models of HHM.
Hypercalcemia was induced either by sc
inoculation of syngeneic colon (C-26)
adenocarcinoma cells or by sc injection of
high-dose recombinant PTHrP (0.5 mg/kg, sc, twice
per day). In both models, OPG (0.25 mg/kg)
caused rapid reversal of established
hypercalcemia, and the speed and duration of
hypercalcemia suppression were significantly
greater with OPG (5 mg/kg) than with high-dose
bisphosphonates (pamidronate or zoledronic acid,
5 mg/kg).
OPG also caused greater reductions in osteoclast
surface and biochemical markers of bone
resorption compared with either bisphosphonate.
In both models, hypercalcemia gradually returned
despite clear evidence of ongoing suppression of
bone resorption by OPG.
These data demonstrate that osteoclasts and RANKL
are important mediators of HHM, particularly in
the early stages of the condition.
Aggressive antiresorptive therapy with a RANKL
inhibitor therefore might be a rational approach
to controlling HHM.

41
Areas of Uncertainty (2)

Preliminary data from studies in animals or small
studies involving women with osteoporosis
indicate reductions in bone resorption with these
approaches.
Whether these agents will prove to be safe and
effective in humans with hypercalcemia associated
with cancer, whether they can be produced
commercially at a cost competitive with that of
bisphosphonates, and whether they can reverse
hypercalcemia more effectively than the potent
bisphosphonates remain unknown.

42
The effect of a single dose of osteoprotegerin in
postmenopausal women

Osteoprotegerin (OPG), a TNF receptor family
member, is a critical regulator of bone
resorption. It is an important inhibitor of the
terminal differentiation and activation of
osteoclasts.
This randomized, double-blind, placebo-controlled,
sequential dose escalation study was conducted
in postmenopausal women to determine the effect
of a single S.C. dose of OPG on bone resorption
as indicated by the biochemical markers, urinary
N-telopeptide (NTX) and deoxypyridinoline (DPD),
which are stable collagen degradation products.
NTX decreased within 12 h after OPG
administration.
At the highest dose administered (3.0 mg/kg), a
mean percent decrease in NTX of 80 was observed
4 days after dosing. Six weeks after dosing a
mean decrease of 14 in NTX was observed.

J Bone Miner Res 200116348-360
43

The bone-specific alkaline phosphatase (BSAP), a
marker of bone formation, did not change for 3
weeks after dosing. Thereafter, a modest
decrease, reaching 30 at 6 weeks, was observed
in the 3.0-mg/kg dose group.
The rapid decrease from baseline in NTX and
delayed decrease in BSAP indicated that OPG acted
primarily on osteoclasts to decrease bone
resorption. OPG injections are well tolerated.
This study, for the first time, indicates that a
single s.c. injection of OPG is effective in
rapidly and profoundly reducing bone turnover for
a sustained period and that OPG therefore may be
effective in Tx of bone diseases characterized by
increased bone resorption such as osteoporosis

44
A single-dose placebo-controlled study of AMG
162, a fully human monoclonal Ab to RANKL, in
postmenopausal women

The safety and bone antiresorptive effect of a
single S.C. dose of AMG 162, a human monoclonal
Ab to RANKL, was investigated in 49
postmenopausal women. AMG 162 is a potent
antiresorptive agent for diseases such as
osteoporosis.
INTRODUCTION RANKL is an essential osteoclastic
differentiation and activation factor.
MATERIALS AND METHODS The bone antiresorptive
activity and safety of AMG 162, a fully human
monoclonal Ab to RANKL, were evaluated in
postmenopausal women in this randomized,
double-blind, placebo-controlled, single-dose,
dose escalation study. Six cohorts of eight to
nine women were randomly assigned to receive a
single S.C. injection of either AMG 162 or
placebo (31 ratio). AMG 162 doses were 0.01,
0.03, 0.1, 0.3, 1.0, and 3.0 mg/kg.Subjects were
followed up to 6 months in all cohorts and 9
months in the three highest dose cohorts. Second
morning void urinary N-telopeptide/Cr (NTX
Osteomark), serum NTX, and serum bone-specific
alkaline phosphatase (BALP, Ostase) were assessed
as bone turnover markers.

J Bone Miner Res 2004191059-1066
45

RESULTS AND CONCLUSIONS Forty-nine women were
enrolled. A single SC dose of AMG 162 resulted in
a dose-dependent, rapid (within 12 h), profound
(up to 84), and sustained (up to 6 months)
decrease in urinary NTX. At 6 months, there was a
mean change from baseline of -81 in the 3.0
mg/kg AMG 162 group compared with -10 in the
placebo group serum NTX changes were -56 and
2, respectively. BALP did not decrease
remarkably until after 1 month, indicating that
the effect of AMG 162 is primarily
antiresorptive. Intact PTH increased up to
3-fold after 4 days in the 3.0 mg/kg dose group,
but returned toward baseline with follow-up.
Alb-adjusted serum Ca did not decrease gt10 on
average in any group, and no subject had values
below 2 mmol/liter. AMG 162 was well tolerated.
No related serious adverse events occurred. No
clinically meaningful laboratory changes, other
than those described above, were observed.
In summary, a single SC dose of AMG 162 resulted
in a dose-dependent rapid and sustained decrease
from baseline in bone turnover and could be an
effective and convenient Tx for osteoporosis.

J Bone Miner Res 2004191059-1066
46
Tx of malignancy-associated hypercalcemia and
cachexia with humanized anti-PTH-related protein
Ab

PTHrP plays a central role in HHM, which is one
of the most frequent paraneoplastic syndromes.
PTHrP produced by the tumor acts through a common
PTH/PTHrP receptor to promote bone resorption,
inhibit Ca excretion from the kidney, and induce
hypercalcemia. P'ts with HHM often develop
cachexia associated with typical symptoms such as
anorexia, malaise, nausea, constipation,
polyuria, polydipsia, and confusion. The etiology
of the cachexia is not fully understood but is
thought to be caused by hypercalcemia and various
cytokines such as IL-6, TNF-alpha, leukemia
inhibitory factor, and others. In this study, we
investigated the role of PTHrP in hypercalcemia
and cachexia in HHM by using humanized anti-PTHrP
Ab.
A mouse monoclonal Ab that binds to PTHrP amino
acid sequence 1-34 and inhibits PTHrP function
has been humanized to create a specific and
potent agent for the Tx of p'ts with HHM. The
mouse monoclonal Ab has been shown to have
antihypercalcemic activity against nude mice
bearing human tumors.

Semin Oncol 200330Suppl 16167-173
47

Because a mouse Ab is highly immunogenic in human
p'ts, the complementarity-determining regions
from the mouse Ab were grafted into a human Ab.
The resulting humanized Ab specifically
recognizes PTHrP(1-34) and neutralizes PTHrP
functions in vitro and in vivo. The humanized
anti-PTHrP Ab was administered IV to HHM model
animals bearing tumors such as LC-6 human lung
carcinoma. These animals showed symptoms similar
to those of p'ts with HHM (eg, hypercalcemia and
cachexia). The humanized anti-PTHrP Ab-treated
animals responded with normalization of blood
ionized Ca through an improvement of bone
metabolism and Ca excretion. Moreover, the
treated animals also showed an improvement in BW,
ultromotivity, metabolic alkalosis, food
consumption, water intake, serum phosphorus, and
renal function. Consequently, the humanized
Ab-treated animals experienced complete
resolution of hypercalcemia and cachexia.
These results suggest that the humanized Ab would
be an effective and beneficial agent for p'ts
with HHM, and that PTHrP is a major pathogenetic
factor of hypercalcemia and cachexia in p'ts with
HHM.

Semin Oncol 200330Suppl 16167-173
48
Guidelines

No guidelines are available from the major
professional societies for the Tx of
hypercalcemia associated with cancer.

49
Recommendations (1)

The p't described in the vignette, who has breast
cancer and a large, obvious tumor burden, is
typical of p'ts with hypercalcemia associated
with cancer in general and with HHM in
particular.
As in all cases of hypercalcemia in p'ts with
cancer, other causes of the hypercalcemia need to
be carefully considered.
Coexisting primary hyperparathyroidism should
routinely be ruled out by measurement of
immunoreactive PTH.
In the p't described, HHM is the most likely
cause of the hypercalcemia thus, immunoreactive
PTH would be suppressed and circulating PTHrP
would be elevated (however, I do not routinely
measure PTHrP unless the Dx is uncertain).

50
Recommendations (2)

When a p't presents with hypercalcemia associated
with cancer, the physician should first consider
whether Tx is appropriate according to an
assessment of the overall prognosis.
The cornerstones of successful antihypercalcemic
therapy are vigorous rehydration (with the use of
NS at 200 to 500 ml /hr, depending on the p't's
CV status and renal function) aggressive
calciuresis with the use of loop diuretics, after
normovolemia has been restored and inhibition of
bone resorption with the use of IV
bisphosphonates (in the USA, the administration
of either pamidronate an infusion of 60 to 90 mg
over a 2-hour period or zoledronate 4 mg over a
15-minute period).

51
Recommendations (3)

Pamidronate is at present less expensive, whereas
zoledronate is more convenient to use and results
in slightly greater mean reductions in the serum
Ca , although the differences are small.
The expectation with the use of either regimen is
that the serum Ca will begin to fall within 12
hours after the therapy is initiated and will
reach the nadir within four to seven days.
The serum Ca generally will remain in the normal
or near-normal range for one to three weeks,
allowing time to institute other Txs for the
malignant disease responsible for the
hypercalcemia.