Date published: 2025-10-25

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hCAP-H Inhibitors

Chemicals classified as hCAP-H inhibitors encompass a range of compounds that interfere with mitotic functions and chromosomal architecture indirectly. These inhibitors do not target hCAP-H directly; rather, they impact the protein's function by altering the cellular processes and signaling pathways that facilitate proper chromosome condensation and segregation during mitosis. Compounds such as Paclitaxel and Vinblastine act on the microtubule network, which is essential for the mitotic spindle assembly. By stabilizing or destabilizing microtubules, these compounds can disrupt the proper function of the spindle apparatus, thereby indirectly affecting the role of hCAP-H in chromosome condensation and stabilization.

Nocodazole and Monastrol exert similar effects by targeting microtubule dynamics and kinesin motors, respectively, which are critical for spindle formation and function. BI 2536 and S-trityl-L-cysteine focus their action on key mitotic kinases like Plk1 and the motor protein Eg5, respectively. Their inhibition leads to defects in spindle assembly and function, which can indirectly inhibit the function of hCAP-H. Aurora kinases are another important target for hCAP-H inhibitors. Compounds such as ZM447439, VX-680, and Alisertib inhibit Aurora kinase activity, which is pivotal for chromosome alignment and segregation. By disrupting these processes, the compounds indirectly affect hCAP-H function, which is crucial for maintaining chromosome architecture during mitosis. Mitoxantrone and Amsacrine target topoisomerase II, which is involved in DNA replication and decatenation, processes that are fundamental for proper chromosome condensation and segregation.

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Items 1 to 10 of 11 total

Display:

Product NameCAS #Catalog #QUANTITYPriceCitationsRATING

Taxol

33069-62-4sc-201439D
sc-201439
sc-201439A
sc-201439E
sc-201439B
sc-201439C
1 mg
5 mg
25 mg
100 mg
250 mg
1 g
$40.00
$73.00
$217.00
$242.00
$724.00
$1196.00
39
(2)

Stabilizes microtubules and disrupts mitotic spindle function, which can indirectly inhibit hCAP-H by interrupting proper chromosome condensation.

Vinblastine

865-21-4sc-491749
sc-491749A
sc-491749B
sc-491749C
sc-491749D
10 mg
50 mg
100 mg
500 mg
1 g
$100.00
$230.00
$450.00
$1715.00
$2900.00
4
(0)

Destabilizes microtubules, impeding spindle formation and thereby indirectly affecting hCAP-H's role in chromosomes during mitosis.

Nocodazole

31430-18-9sc-3518B
sc-3518
sc-3518C
sc-3518A
5 mg
10 mg
25 mg
50 mg
$58.00
$83.00
$140.00
$242.00
38
(2)

Disrupts microtubule polymerization, which can interfere with mitotic spindle function and indirectly inhibit hCAP-H activity.

Monastrol

254753-54-3sc-202710
sc-202710A
1 mg
5 mg
$120.00
$233.00
10
(1)

Inhibits the kinesin Eg5, which is essential for bipolar spindle assembly, possibly affecting hCAP-H function during chromosome segregation.

BI6727

755038-65-4sc-364432
sc-364432A
sc-364432B
sc-364432C
sc-364432D
5 mg
50 mg
100 mg
500 mg
1 g
$147.00
$1029.00
$1632.00
$3264.00
$4296.00
1
(1)

Inhibits Polo-like kinase 1 (Plk1), a key regulator of mitosis, potentially affecting hCAP-H's involvement in chromosome architecture.

S-Trityl-L-cysteine

2799-07-7sc-202799
sc-202799A
1 g
5 g
$31.00
$65.00
6
(1)

Inhibits mitotic kinesin Eg5, leading to monopolar spindle formation and indirect inhibition of hCAP-H's role in mitosis.

ZM-447439

331771-20-1sc-200696
sc-200696A
1 mg
10 mg
$150.00
$349.00
15
(1)

Inhibits Aurora kinase activity, which is essential for chromosome alignment and segregation, potentially affecting hCAP-H function.

Tozasertib

639089-54-6sc-358750
sc-358750A
25 mg
50 mg
$61.00
$85.00
4
(1)

Inhibits Aurora kinases, which are necessary for proper chromosome segregation, thus indirectly inhibiting hCAP-H activity.

MLN8237

1028486-01-2sc-394162
5 mg
$220.00
(0)

Inhibits Aurora A kinase, affecting chromosome alignment and indirectly influencing hCAP-H's role in chromosomal condensation.

Mitoxantrone

65271-80-9sc-207888
100 mg
$279.00
8
(1)

Interferes with topoisomerase II, which is involved in DNA replication and decatenation, indirectly affecting hCAP-H activity.